TY  - CHAP
AU  - Medarević, Đorđe
AU  - Krstić, Mirjana
AU  - Ibrić, Svetlana
PY  - 2024
UR  - https://farfar.pharmacy.bg.ac.rs/handle/123456789/5607
AB  - With the progress in medicine during the last several decades, it became clear
that the course of the disease and response to applied therapy differ to a great
extent between patients due to differences in genetic, anatomical, and physiological
characteristics of the patients. This brought into question the current
concept of therapy, so-called one size fits all, where similar drug doses have
been prescribed to a huge number of patients, with neglect of interindividual
differences between patients.
PB  - Elsevier Inc.
T2  - From Current to Future Trends in Pharmaceutical Technology
T1  - Fundamentals of 3D printing of pharmaceuticals
SP  - 1
EP  - 65
DO  - 10.1016/B978-0-323-91111-5.00001-9
ER  - 

@inbook{
author = "Medarević, Đorđe and Krstić, Mirjana and Ibrić, Svetlana",
year = "2024",
abstract = "With the progress in medicine during the last several decades, it became clear
that the course of the disease and response to applied therapy differ to a great
extent between patients due to differences in genetic, anatomical, and physiological
characteristics of the patients. This brought into question the current
concept of therapy, so-called one size fits all, where similar drug doses have
been prescribed to a huge number of patients, with neglect of interindividual
differences between patients.",
publisher = "Elsevier Inc.",
journal = "From Current to Future Trends in Pharmaceutical Technology",
booktitle = "Fundamentals of 3D printing of pharmaceuticals",
pages = "1-65",
doi = "10.1016/B978-0-323-91111-5.00001-9"
}

Medarević, Đ., Krstić, M.,& Ibrić, S.. (2024). Fundamentals of 3D printing of pharmaceuticals. in From Current to Future Trends in Pharmaceutical Technology
Elsevier Inc.., 1-65.
https://doi.org/10.1016/B978-0-323-91111-5.00001-9

Medarević Đ, Krstić M, Ibrić S. Fundamentals of 3D printing of pharmaceuticals. in From Current to Future Trends in Pharmaceutical Technology. 2024;:1-65.
doi:10.1016/B978-0-323-91111-5.00001-9 .

Medarević, Đorđe, Krstić, Mirjana, Ibrić, Svetlana, "Fundamentals of 3D printing of pharmaceuticals" in From Current to Future Trends in Pharmaceutical Technology (2024):1-65,
https://doi.org/10.1016/B978-0-323-91111-5.00001-9 . .

TY  - CONF
AU  - Medarević, Đorđe
AU  - Turković, Erna
AU  - Čežek, Maša
AU  - Ibrić, Svetlana
AU  - Maksimović, Zoran
PY  - 2024
UR  - https://farfar.pharmacy.bg.ac.rs/handle/123456789/5606
AB  - INTRODUCTION
Crop residues (CRs) represent a resource that is available in
virtually unlimited quantities, but still the largest part
remains unused. Unfortunately, CRs are usually burned in
the field, which causes air pollution, contributes to global
warming by emitting greenhouse gasses, hinders nutrient
recycling, and negatively affects soil microbes through
overheating and carbon loss [1]. One of the most important
value-added components that can be isolated from CRs is
microcrystalline cellulose (MCC), a common excipient in
tablet formulation. In this study, a comparative evaluation
of tableting properties of MCC obtained from wheat and
corn CRs by different chemical treatment was performed. ...
PB  - International Association for Pharmaceutical Technology (APV), Mainz, Germany
PB  - International Society of Drug Delivery Sciences and Technology (APGI), Lille, France
PB  - Italian Society of Technology and Legislation (S.I.T.E.L.F), Milan, Italy
C3  - 14th World Meeting on Pharmaceutics, Biopharmaceutics and Pharmaceutical Technology, 18 - 21 March 2024, Vienna, Austria
T1  - Comparative evaluation of tableting properties of microcrystalline cellulose obtained from wheat and corn crop residues
UR  - https://hdl.handle.net/21.15107/rcub_farfar_5606
ER  - 

@conference{
author = "Medarević, Đorđe and Turković, Erna and Čežek, Maša and Ibrić, Svetlana and Maksimović, Zoran",
year = "2024",
abstract = "INTRODUCTION
Crop residues (CRs) represent a resource that is available in
virtually unlimited quantities, but still the largest part
remains unused. Unfortunately, CRs are usually burned in
the field, which causes air pollution, contributes to global
warming by emitting greenhouse gasses, hinders nutrient
recycling, and negatively affects soil microbes through
overheating and carbon loss [1]. One of the most important
value-added components that can be isolated from CRs is
microcrystalline cellulose (MCC), a common excipient in
tablet formulation. In this study, a comparative evaluation
of tableting properties of MCC obtained from wheat and
corn CRs by different chemical treatment was performed. ...",
publisher = "International Association for Pharmaceutical Technology (APV), Mainz, Germany, International Society of Drug Delivery Sciences and Technology (APGI), Lille, France, Italian Society of Technology and Legislation (S.I.T.E.L.F), Milan, Italy",
journal = "14th World Meeting on Pharmaceutics, Biopharmaceutics and Pharmaceutical Technology, 18 - 21 March 2024, Vienna, Austria",
title = "Comparative evaluation of tableting properties of microcrystalline cellulose obtained from wheat and corn crop residues",
url = "https://hdl.handle.net/21.15107/rcub_farfar_5606"
}

Medarević, Đ., Turković, E., Čežek, M., Ibrić, S.,& Maksimović, Z.. (2024). Comparative evaluation of tableting properties of microcrystalline cellulose obtained from wheat and corn crop residues. in 14th World Meeting on Pharmaceutics, Biopharmaceutics and Pharmaceutical Technology, 18 - 21 March 2024, Vienna, Austria
International Association for Pharmaceutical Technology (APV), Mainz, Germany..
https://hdl.handle.net/21.15107/rcub_farfar_5606

Medarević Đ, Turković E, Čežek M, Ibrić S, Maksimović Z. Comparative evaluation of tableting properties of microcrystalline cellulose obtained from wheat and corn crop residues. in 14th World Meeting on Pharmaceutics, Biopharmaceutics and Pharmaceutical Technology, 18 - 21 March 2024, Vienna, Austria. 2024;.
https://hdl.handle.net/21.15107/rcub_farfar_5606 .

Medarević, Đorđe, Turković, Erna, Čežek, Maša, Ibrić, Svetlana, Maksimović, Zoran, "Comparative evaluation of tableting properties of microcrystalline cellulose obtained from wheat and corn crop residues" in 14th World Meeting on Pharmaceutics, Biopharmaceutics and Pharmaceutical Technology, 18 - 21 March 2024, Vienna, Austria (2024),
https://hdl.handle.net/21.15107/rcub_farfar_5606 .

TY  - CONF
AU  - Medarević, Đorđe
AU  - Čežek, Maša
AU  - Knežević, Aleksandar
AU  - Pešić, Nikola
AU  - Ibrić, Svetlana
AU  - Maksimović, Zoran
PY  - 2023
UR  - https://farfar.pharmacy.bg.ac.rs/handle/123456789/5070
AB  - Crop residues (CR) are usually burned in the field,
which causes air pollution, contributes to global warming,
hinders nutrient recycling, and negatively affects soil
microbes through overheating and carbon loss. There is
growing interest in developing processes for isolation of
value added components with application in different
industries from CR as feedstock. In this study, different
procedures for isolation of microcrystalline cellulose
(MCC) from wheat, corn and sunflower CR were
evaluated, with further testing of functional characteristics
of MCC, which are relevant for tablets production.
PB  - Macedonian Pharmaceutical Association
PB  - Ss. Cyril and Methodius University in Skopje, Faculty of Pharmacy
C3  - Macedonian Pharmaceutical Bulletin
T1  - Functional characterization of microcrystalline cellulose obtained from the crop residues
VL  - 69
IS  - Suppl 1
SP  - 185
EP  - 186
DO  - 10.33320/maced.pharm.bull.2023.69.03.091
ER  - 

@conference{
author = "Medarević, Đorđe and Čežek, Maša and Knežević, Aleksandar and Pešić, Nikola and Ibrić, Svetlana and Maksimović, Zoran",
year = "2023",
abstract = "Crop residues (CR) are usually burned in the field,
which causes air pollution, contributes to global warming,
hinders nutrient recycling, and negatively affects soil
microbes through overheating and carbon loss. There is
growing interest in developing processes for isolation of
value added components with application in different
industries from CR as feedstock. In this study, different
procedures for isolation of microcrystalline cellulose
(MCC) from wheat, corn and sunflower CR were
evaluated, with further testing of functional characteristics
of MCC, which are relevant for tablets production.",
publisher = "Macedonian Pharmaceutical Association, Ss. Cyril and Methodius University in Skopje, Faculty of Pharmacy",
journal = "Macedonian Pharmaceutical Bulletin",
title = "Functional characterization of microcrystalline cellulose obtained from the crop residues",
volume = "69",
number = "Suppl 1",
pages = "185-186",
doi = "10.33320/maced.pharm.bull.2023.69.03.091"
}

Medarević, Đ., Čežek, M., Knežević, A., Pešić, N., Ibrić, S.,& Maksimović, Z.. (2023). Functional characterization of microcrystalline cellulose obtained from the crop residues. in Macedonian Pharmaceutical Bulletin
Macedonian Pharmaceutical Association., 69(Suppl 1), 185-186.
https://doi.org/10.33320/maced.pharm.bull.2023.69.03.091

Medarević Đ, Čežek M, Knežević A, Pešić N, Ibrić S, Maksimović Z. Functional characterization of microcrystalline cellulose obtained from the crop residues. in Macedonian Pharmaceutical Bulletin. 2023;69(Suppl 1):185-186.
doi:10.33320/maced.pharm.bull.2023.69.03.091 .

Medarević, Đorđe, Čežek, Maša, Knežević, Aleksandar, Pešić, Nikola, Ibrić, Svetlana, Maksimović, Zoran, "Functional characterization of microcrystalline cellulose obtained from the crop residues" in Macedonian Pharmaceutical Bulletin, 69, no. Suppl 1 (2023):185-186,
https://doi.org/10.33320/maced.pharm.bull.2023.69.03.091 . .

TY  - CONF
AU  - Adamov, Ivana
AU  - Medarević, Đorđe
AU  - Pešić, Nikola
AU  - Ivković, Branka
AU  - Kočović, David
AU  - Grujić, Branka
AU  - Ibrić, Svetlana
PY  - 2023
UR  - https://farfar.pharmacy.bg.ac.rs/handle/123456789/5335
AB  - Trodimenzionalna (3D) štampa predstavlja inovativnu tehnologiju u oblasti farmacije, koja ima potencijal da obezbedi proizvodnju malih serija lekova prilagođenih individualnim potrebama pacijenata. Intenzivno istraživanje u oblasti 3D štampe rezultovalo je razvojem velikog broj različitih tehnika, a čija osnovna, zajednička karakteristika jeste štampanje u slojevima. ...
AB  - Three-dimensional (3D) printing is an innovative technology in the field of pharmacy with potential to provide manufacturing of small batches of patient-taiIored medicines. Intensive research in the field of 3D printing has resulted in development of numerous different techniques whose common feature is printing in layers The aim of this study was to formulate and comparatively characterize orodispersible tablets (ODTs) of desloratadine (DSL) obtained by 3D selective laser sintering (SLS) technique with commercially available ODTs. ...
PB  - Farmaceutska komora Crne Gore
PB  - Univerzitet Crne Gore, Medicinski fakultet, studijski program-farmacija
C3  - 4. kongres farmaceuta Crne Gore sa međunarodnim učešćem, 11-14. maj 2023. Budva, Bečići, Crna Gora, Zbornik sažetaka
T1  - Formulacija i karakterizacija oralno-disperzibilnih tableta desloratadina dobijenih 3D tehnikom selektivnog laserskog sinterovanja
VL  - PP-12
SP  - 104
EP  - 105
UR  - https://hdl.handle.net/21.15107/rcub_farfar_5335
ER  - 

@conference{
author = "Adamov, Ivana and Medarević, Đorđe and Pešić, Nikola and Ivković, Branka and Kočović, David and Grujić, Branka and Ibrić, Svetlana",
year = "2023",
abstract = "Trodimenzionalna (3D) štampa predstavlja inovativnu tehnologiju u oblasti farmacije, koja ima potencijal da obezbedi proizvodnju malih serija lekova prilagođenih individualnim potrebama pacijenata. Intenzivno istraživanje u oblasti 3D štampe rezultovalo je razvojem velikog broj različitih tehnika, a čija osnovna, zajednička karakteristika jeste štampanje u slojevima. ..., Three-dimensional (3D) printing is an innovative technology in the field of pharmacy with potential to provide manufacturing of small batches of patient-taiIored medicines. Intensive research in the field of 3D printing has resulted in development of numerous different techniques whose common feature is printing in layers The aim of this study was to formulate and comparatively characterize orodispersible tablets (ODTs) of desloratadine (DSL) obtained by 3D selective laser sintering (SLS) technique with commercially available ODTs. ...",
publisher = "Farmaceutska komora Crne Gore, Univerzitet Crne Gore, Medicinski fakultet, studijski program-farmacija",
journal = "4. kongres farmaceuta Crne Gore sa međunarodnim učešćem, 11-14. maj 2023. Budva, Bečići, Crna Gora, Zbornik sažetaka",
title = "Formulacija i karakterizacija oralno-disperzibilnih tableta desloratadina dobijenih 3D tehnikom selektivnog laserskog sinterovanja",
volume = "PP-12",
pages = "104-105",
url = "https://hdl.handle.net/21.15107/rcub_farfar_5335"
}

Adamov, I., Medarević, Đ., Pešić, N., Ivković, B., Kočović, D., Grujić, B.,& Ibrić, S.. (2023). Formulacija i karakterizacija oralno-disperzibilnih tableta desloratadina dobijenih 3D tehnikom selektivnog laserskog sinterovanja. in 4. kongres farmaceuta Crne Gore sa međunarodnim učešćem, 11-14. maj 2023. Budva, Bečići, Crna Gora, Zbornik sažetaka
Farmaceutska komora Crne Gore., PP-12, 104-105.
https://hdl.handle.net/21.15107/rcub_farfar_5335

Adamov I, Medarević Đ, Pešić N, Ivković B, Kočović D, Grujić B, Ibrić S. Formulacija i karakterizacija oralno-disperzibilnih tableta desloratadina dobijenih 3D tehnikom selektivnog laserskog sinterovanja. in 4. kongres farmaceuta Crne Gore sa međunarodnim učešćem, 11-14. maj 2023. Budva, Bečići, Crna Gora, Zbornik sažetaka. 2023;PP-12:104-105.
https://hdl.handle.net/21.15107/rcub_farfar_5335 .

Adamov, Ivana, Medarević, Đorđe, Pešić, Nikola, Ivković, Branka, Kočović, David, Grujić, Branka, Ibrić, Svetlana, "Formulacija i karakterizacija oralno-disperzibilnih tableta desloratadina dobijenih 3D tehnikom selektivnog laserskog sinterovanja" in 4. kongres farmaceuta Crne Gore sa međunarodnim učešćem, 11-14. maj 2023. Budva, Bečići, Crna Gora, Zbornik sažetaka, PP-12 (2023):104-105,
https://hdl.handle.net/21.15107/rcub_farfar_5335 .

TY  - CONF
AU  - Adamov, Ivana
AU  - Glišić, Teodora
AU  - Medarević, Đorđe
AU  - Aleksić, Ivana
AU  - Ibrić, Svetlana
PY  - 2023
UR  - https://farfar.pharmacy.bg.ac.rs/handle/123456789/5331
AB  - 3D štampa lekova, kao aditivna tehnologija, predstavlja jednostavnu i ekonomski prihvatljivu
alternativu konvencionalnim metodama, pružajući mogućnost dobijanja inovativnih farmaceutskih
oblika i prilagođavanje terapije individualnim potrebama pacijenata (1). Cilj istraživanja bio je da se
formulišu i izrade mini tablete desloratadinа (DSL) primenom 3D tehnike digitalne obrade svetlosti
(engl. Digital light processing, DLP) mehanizmom nanošenja materijala “sloj po sloj”. Mini tablete DSL
(10%, m/m) odabrane su kao farmaceutski oblik leka koji je pogodan za primenu u pedijatrijskoj
populaciji, pre svega sa aspekta fleksibilnosti doziranja. Pripremljena je formulacija sa 1%
fotoinicijatora i 10% vode, dok su polietilenglikol-diakrilat i polietilenglikol 400 bili prisutni u
masenom odnosu 1:1. Kreirani 3D modeli (4,00 × 3,00 mm) uspešno su odštampani primenom
WanhaoD8 štampača. Dobijene su žuto-narandžaste mini tablete uniformnog oblika, debljine i mase
(4,16 ± 0,06 × 2,24 ± 0,04 mm; 42,61 ± 1,15 mg). Nepotpuna ekstrakcija DSL iz unakrsno umreženog
polimernog matriksa rezultovala je relativno niskim sadržajem lekovite supstance u mini tabletama
u odnosu na teorijski sadržaj (72,14 ± 1,04%) (2). Prilikom ispitivanja brzine rastvaranja, nakon 45
min oslobođeno je 50,29 ± 0,14% DSL u 0,1M hlorovodoničnoj kiselini, kao medijumu, uz postizanje
platoa nakon 4 sata (81,19 ± 0,63%). Rezultati DSC analize pokazali su da je došlo do amorfizacije
lekovite supstance, dok je posmatranjem poprečnih preseka odštampanih mini tableta pod
polarizacionim svetlosnim mikroskopom uočeno prisustvo slojevite strukture. DLP tehnika 3D
štampe lekova ima potencijal da obezbedi brzu izradu mini tableta odgovarajućih fizičko-hemijskih
karakteristika, uz mogućnost postizanja modifikovanog oslobađanja lekovite supstance.
AB  - 3D printing as an additive technology represents a simple and economically acceptable
alternative to conventional methods and offers the possibility of obtaining innovative dosage forms
and individualizing therapy according to the specific needs of patients. (1). The aim of the research
was to formulate and manufacture desloratadine mini-tablets (DSL) using digital light processing
(DLP) 3D technique based on a successive layering mechanism. Mini-tablets of DSL (10%,w/w) were
selected as a dosage form suitable for the pediatric population, particularly because of its flexible
dosing. The formulation was prepared with 1% photoinitiator and 10% water, while poly(ethylene
glycol) diacrylate and poly(ethylene glycol) 400 were present in a mass ratio of 1:1. The created 3D
models (4.00×3.00 mm) were successfully printed using WanhaoD8 printer. Yellow-orange mini-
tablets with uniform shape, thickness and mass (4.16±0.06×2.24±0.04 mm; 42.61±1.15 mg) were
produced. Incomplete extraction of DSL from the cross-linked polymer matrix resulted in a relatively
low content of the drug in the mini-tablets compared to the theoretical content (72.14±1.04%) (2).
The dissolution test showed that 50.29±0.14% of DSL was released after 45 minutes in 0.1M
hydrochloric acid medium and reached a plateau after 4 hours (81.19±0.63%). The results of DSC
analysis showed amorphisation of the drug, while observation of the cross-sections of printed mini-
tablets under a polarizing microscope indicated the presence of a layered structure. The DLP
technique has the potential to ensure the rapid production of mini-tablets with suitable
physicochemical properties and to enable modified release of the drug.
PB  - Savez farmaceutskih udruženja Srbije
C3  - Arhiv za farmaciju
T1  - Formulacija i karakterizacija mini tableta desloratadina dobijenih  fotopolimerizacionom tehnikom 3D štampe lekova
T1  - Formulation and characterization of desloratadine mini-tablets obtained by photopolimerization 3D printing technique
VL  - 73
IS  - Suppl. 4
SP  - S59
EP  - S60
UR  - https://hdl.handle.net/21.15107/rcub_farfar_5331
ER  - 

@conference{
author = "Adamov, Ivana and Glišić, Teodora and Medarević, Đorđe and Aleksić, Ivana and Ibrić, Svetlana",
year = "2023",
abstract = "3D štampa lekova, kao aditivna tehnologija, predstavlja jednostavnu i ekonomski prihvatljivu
alternativu konvencionalnim metodama, pružajući mogućnost dobijanja inovativnih farmaceutskih
oblika i prilagođavanje terapije individualnim potrebama pacijenata (1). Cilj istraživanja bio je da se
formulišu i izrade mini tablete desloratadinа (DSL) primenom 3D tehnike digitalne obrade svetlosti
(engl. Digital light processing, DLP) mehanizmom nanošenja materijala “sloj po sloj”. Mini tablete DSL
(10%, m/m) odabrane su kao farmaceutski oblik leka koji je pogodan za primenu u pedijatrijskoj
populaciji, pre svega sa aspekta fleksibilnosti doziranja. Pripremljena je formulacija sa 1%
fotoinicijatora i 10% vode, dok su polietilenglikol-diakrilat i polietilenglikol 400 bili prisutni u
masenom odnosu 1:1. Kreirani 3D modeli (4,00 × 3,00 mm) uspešno su odštampani primenom
WanhaoD8 štampača. Dobijene su žuto-narandžaste mini tablete uniformnog oblika, debljine i mase
(4,16 ± 0,06 × 2,24 ± 0,04 mm; 42,61 ± 1,15 mg). Nepotpuna ekstrakcija DSL iz unakrsno umreženog
polimernog matriksa rezultovala je relativno niskim sadržajem lekovite supstance u mini tabletama
u odnosu na teorijski sadržaj (72,14 ± 1,04%) (2). Prilikom ispitivanja brzine rastvaranja, nakon 45
min oslobođeno je 50,29 ± 0,14% DSL u 0,1M hlorovodoničnoj kiselini, kao medijumu, uz postizanje
platoa nakon 4 sata (81,19 ± 0,63%). Rezultati DSC analize pokazali su da je došlo do amorfizacije
lekovite supstance, dok je posmatranjem poprečnih preseka odštampanih mini tableta pod
polarizacionim svetlosnim mikroskopom uočeno prisustvo slojevite strukture. DLP tehnika 3D
štampe lekova ima potencijal da obezbedi brzu izradu mini tableta odgovarajućih fizičko-hemijskih
karakteristika, uz mogućnost postizanja modifikovanog oslobađanja lekovite supstance., 3D printing as an additive technology represents a simple and economically acceptable
alternative to conventional methods and offers the possibility of obtaining innovative dosage forms
and individualizing therapy according to the specific needs of patients. (1). The aim of the research
was to formulate and manufacture desloratadine mini-tablets (DSL) using digital light processing
(DLP) 3D technique based on a successive layering mechanism. Mini-tablets of DSL (10%,w/w) were
selected as a dosage form suitable for the pediatric population, particularly because of its flexible
dosing. The formulation was prepared with 1% photoinitiator and 10% water, while poly(ethylene
glycol) diacrylate and poly(ethylene glycol) 400 were present in a mass ratio of 1:1. The created 3D
models (4.00×3.00 mm) were successfully printed using WanhaoD8 printer. Yellow-orange mini-
tablets with uniform shape, thickness and mass (4.16±0.06×2.24±0.04 mm; 42.61±1.15 mg) were
produced. Incomplete extraction of DSL from the cross-linked polymer matrix resulted in a relatively
low content of the drug in the mini-tablets compared to the theoretical content (72.14±1.04%) (2).
The dissolution test showed that 50.29±0.14% of DSL was released after 45 minutes in 0.1M
hydrochloric acid medium and reached a plateau after 4 hours (81.19±0.63%). The results of DSC
analysis showed amorphisation of the drug, while observation of the cross-sections of printed mini-
tablets under a polarizing microscope indicated the presence of a layered structure. The DLP
technique has the potential to ensure the rapid production of mini-tablets with suitable
physicochemical properties and to enable modified release of the drug.",
publisher = "Savez farmaceutskih udruženja Srbije",
journal = "Arhiv za farmaciju",
title = "Formulacija i karakterizacija mini tableta desloratadina dobijenih  fotopolimerizacionom tehnikom 3D štampe lekova, Formulation and characterization of desloratadine mini-tablets obtained by photopolimerization 3D printing technique",
volume = "73",
number = "Suppl. 4",
pages = "S59-S60",
url = "https://hdl.handle.net/21.15107/rcub_farfar_5331"
}

Adamov, I., Glišić, T., Medarević, Đ., Aleksić, I.,& Ibrić, S.. (2023). Formulacija i karakterizacija mini tableta desloratadina dobijenih  fotopolimerizacionom tehnikom 3D štampe lekova. in Arhiv za farmaciju
Savez farmaceutskih udruženja Srbije., 73(Suppl. 4), S59-S60.
https://hdl.handle.net/21.15107/rcub_farfar_5331

Adamov I, Glišić T, Medarević Đ, Aleksić I, Ibrić S. Formulacija i karakterizacija mini tableta desloratadina dobijenih  fotopolimerizacionom tehnikom 3D štampe lekova. in Arhiv za farmaciju. 2023;73(Suppl. 4):S59-S60.
https://hdl.handle.net/21.15107/rcub_farfar_5331 .

Adamov, Ivana, Glišić, Teodora, Medarević, Đorđe, Aleksić, Ivana, Ibrić, Svetlana, "Formulacija i karakterizacija mini tableta desloratadina dobijenih  fotopolimerizacionom tehnikom 3D štampe lekova" in Arhiv za farmaciju, 73, no. Suppl. 4 (2023):S59-S60,
https://hdl.handle.net/21.15107/rcub_farfar_5331 .

TY  - CONF
AU  - Pešić, Nikola
AU  - Krkobabić, Mirjana
AU  - Adamov, Ivana
AU  - Ivković, Branka
AU  - Ibrić, Svetlana
AU  - Mirković, Dušica
AU  - Medarević, Đorđe
PY  - 2023
UR  - https://farfar.pharmacy.bg.ac.rs/handle/123456789/5069
AB  - The adjustment of the dose according to the individual
needs of the patient is a unique advantage of 3D printing
technology, which is of particular importance for the
pediatric and geriatric population, due to the diverse needs
and characteristics of these groups of patients (Kotta et al.,
2018).
Selective laser sintering (SLS) is one of the newest 3D
printing techniques that uses powder materials, where the
powder particles are connected under the influence of laser
beams. The main disadvantage of SLS 3D printing is the
high process temperature, which can lead to the
degradation of active substances. On the other hand, this
technique has many advantages, such as high resolution,
the possibility of powder recycling and the absence of pre-
processing (Fina et al., 2018; Thakkar et al., 2021).
PB  - Macedonian Pharmaceutical Association
PB  - Ss. Cyril and Methodius University in Skopje, Faculty of Pharmacy
C3  - Macedonian Pharmaceutical Bulletin
T1  - 3D printing of carvedilol oral dosage forms using selective laser sintering technique
VL  - 69
IS  - Suppl 1
SP  - 169
EP  - 170
DO  - 10.33320/maced.pharm.bull.2023.69.03.083
ER  - 

@conference{
author = "Pešić, Nikola and Krkobabić, Mirjana and Adamov, Ivana and Ivković, Branka and Ibrić, Svetlana and Mirković, Dušica and Medarević, Đorđe",
year = "2023",
abstract = "The adjustment of the dose according to the individual
needs of the patient is a unique advantage of 3D printing
technology, which is of particular importance for the
pediatric and geriatric population, due to the diverse needs
and characteristics of these groups of patients (Kotta et al.,
2018).
Selective laser sintering (SLS) is one of the newest 3D
printing techniques that uses powder materials, where the
powder particles are connected under the influence of laser
beams. The main disadvantage of SLS 3D printing is the
high process temperature, which can lead to the
degradation of active substances. On the other hand, this
technique has many advantages, such as high resolution,
the possibility of powder recycling and the absence of pre-
processing (Fina et al., 2018; Thakkar et al., 2021).",
publisher = "Macedonian Pharmaceutical Association, Ss. Cyril and Methodius University in Skopje, Faculty of Pharmacy",
journal = "Macedonian Pharmaceutical Bulletin",
title = "3D printing of carvedilol oral dosage forms using selective laser sintering technique",
volume = "69",
number = "Suppl 1",
pages = "169-170",
doi = "10.33320/maced.pharm.bull.2023.69.03.083"
}

Pešić, N., Krkobabić, M., Adamov, I., Ivković, B., Ibrić, S., Mirković, D.,& Medarević, Đ.. (2023). 3D printing of carvedilol oral dosage forms using selective laser sintering technique. in Macedonian Pharmaceutical Bulletin
Macedonian Pharmaceutical Association., 69(Suppl 1), 169-170.
https://doi.org/10.33320/maced.pharm.bull.2023.69.03.083

Pešić N, Krkobabić M, Adamov I, Ivković B, Ibrić S, Mirković D, Medarević Đ. 3D printing of carvedilol oral dosage forms using selective laser sintering technique. in Macedonian Pharmaceutical Bulletin. 2023;69(Suppl 1):169-170.
doi:10.33320/maced.pharm.bull.2023.69.03.083 .

Pešić, Nikola, Krkobabić, Mirjana, Adamov, Ivana, Ivković, Branka, Ibrić, Svetlana, Mirković, Dušica, Medarević, Đorđe, "3D printing of carvedilol oral dosage forms using selective laser sintering technique" in Macedonian Pharmaceutical Bulletin, 69, no. Suppl 1 (2023):169-170,
https://doi.org/10.33320/maced.pharm.bull.2023.69.03.083 . .

TY  - JOUR
AU  - Ćirić, Ana
AU  - Milinković Budinčić, Jelena
AU  - Medarević, Đorđe
AU  - Dobričić, Vladimir
AU  - Rmandić, Milena
AU  - Barudžija, Tanja
AU  - Malenović, Anđelija
AU  - Petrović, Lidija
AU  - Đekić, Ljiljana
PY  - 2022
UR  - https://farfar.pharmacy.bg.ac.rs/handle/123456789/4179
AB  - Polyelectrolyte complexes (PECs) are attractive carriers with recognized potential to
enhance oral delivery of poorly soluble high-dosed low-molecular-weight drugs. The formulation
of solid oral dosage forms requires the drying of PECs, which may affect their physicochemical
and biopharmaceutical properties. The aim of this study was to investigate the effect of spray-
drying on the properties of ibuprofen-loaded chitosan/xanthan gum PECs and to assess the drug
release kinetics from such PECs filled into hard capsules in comparison with corresponding PECs
which are dried under ambient conditions. The yield, ibuprofen content, entrapment efficiency,
and residual moisture content of spray-dried PECs were lower than those of ambient-dried PECs.
Better flowability of spray-dried PECs was attributed to the almost spherical particle shape,
shown by scanning electron microscopy. DSC and PXRD analysis confirmed the amorphization
of ibuprofen during spray-drying. All the investigated PECs, obtained by drying under ambient
conditions as well as by spray-drying, had high rehydration capacity both in 0.1 M hydrochloric
acid (pH 1.2) and phosphate buffer pH 7.4. In vitro ibuprofen release from dried PECs was
controlled during 12 h with the release of approximately 30% of entrapped ibuprofen. Spray-dried
PECs provided better control of ibuprofen diffusion from the carrier compared to the ambient-
dried ones.
AB  - Polielektrolitni kompleksi (PEK) su atraktivni nosači sa potencijalom poboljšanja peroralne isporuke slabo rastvorljivih visokodoziranih lekovitih supstanci niske molekulske mase. Formulisanje čvrstih oralnih farmaceutskih oblika na bazi PEK zahteva njihovo sušenje, što može uticati na fizičko-hemijska i biofarmaceutska svojstva kompleksa. Cilj ove studije bio je da se ispita efekat sušenja raspršivanjem na svojstva PEK hitozana i ksantan gume u koje je inkorporiran ibuprofen i da se proceni kinetika oslobađanja lekovite supstance iz takvih PEK napunjenih u tvrde kapsule u poređenju sa odgovarajućim PEK koji su sušeni pod ambijentalnim uslovima. Prinos, sadržaj ibuprofena, efikasnost inkorporiranja i sadržaj vlage PEK sušenih raspršivanjem bili su niži nego kod PEK sušenih pod ambijentalnim uslovima. Bolja protočnost PEK osušenih raspršivanjem je posledica skoro sfernog oblika čestica, što je pokazano skenirajućom elektronskom mikroskopijom. Rezultati DSC i PXRD analiza su potvrdili amorfizaciju ibuprofena tokom sušenja raspršivanjem. Ispitivani PEK osušeni pod različitim uslovima imali su visoku sposobnost rehidratacije u 0,1 M hlorovodoničnoj kiselini (pH 1,2) i fosfatnom puferu pH 7,4. In vitro oslobađanje ibuprofena iz osušenih PEK bilo je kontrolisano tokom 12 h uz oslobađanje približno 30% inkorporiranog ibuprofena. PEK sušeni raspršivanjem obezbedili su bolju kontrolu difuzije ibuprofena iz nosača u poređenju sa onima sušenim pod ambijentalnim uslovima.
PB  - Savez farmaceutskih udruženja Srbije
T2  - Arhiv za farmaciju
T1  - Influence of spray-drying process on properties of chitosan/xanthan gum polyelectrolyte complexes as carriers for oral delivery of ibuprofen
T1  - Uticaj postupka sušenja raspršivanjem na svojstva polielektrolitnih kompleksa hitozana i ksantan gume kao nosača za peroralnu isporuku ibuprofena
VL  - 72
IS  - 1
SP  - 36
EP  - 60
DO  - 10.5937/arhfarm72-35133
ER  - 

@article{
author = "Ćirić, Ana and Milinković Budinčić, Jelena and Medarević, Đorđe and Dobričić, Vladimir and Rmandić, Milena and Barudžija, Tanja and Malenović, Anđelija and Petrović, Lidija and Đekić, Ljiljana",
year = "2022",
abstract = "Polyelectrolyte complexes (PECs) are attractive carriers with recognized potential to
enhance oral delivery of poorly soluble high-dosed low-molecular-weight drugs. The formulation
of solid oral dosage forms requires the drying of PECs, which may affect their physicochemical
and biopharmaceutical properties. The aim of this study was to investigate the effect of spray-
drying on the properties of ibuprofen-loaded chitosan/xanthan gum PECs and to assess the drug
release kinetics from such PECs filled into hard capsules in comparison with corresponding PECs
which are dried under ambient conditions. The yield, ibuprofen content, entrapment efficiency,
and residual moisture content of spray-dried PECs were lower than those of ambient-dried PECs.
Better flowability of spray-dried PECs was attributed to the almost spherical particle shape,
shown by scanning electron microscopy. DSC and PXRD analysis confirmed the amorphization
of ibuprofen during spray-drying. All the investigated PECs, obtained by drying under ambient
conditions as well as by spray-drying, had high rehydration capacity both in 0.1 M hydrochloric
acid (pH 1.2) and phosphate buffer pH 7.4. In vitro ibuprofen release from dried PECs was
controlled during 12 h with the release of approximately 30% of entrapped ibuprofen. Spray-dried
PECs provided better control of ibuprofen diffusion from the carrier compared to the ambient-
dried ones., Polielektrolitni kompleksi (PEK) su atraktivni nosači sa potencijalom poboljšanja peroralne isporuke slabo rastvorljivih visokodoziranih lekovitih supstanci niske molekulske mase. Formulisanje čvrstih oralnih farmaceutskih oblika na bazi PEK zahteva njihovo sušenje, što može uticati na fizičko-hemijska i biofarmaceutska svojstva kompleksa. Cilj ove studije bio je da se ispita efekat sušenja raspršivanjem na svojstva PEK hitozana i ksantan gume u koje je inkorporiran ibuprofen i da se proceni kinetika oslobađanja lekovite supstance iz takvih PEK napunjenih u tvrde kapsule u poređenju sa odgovarajućim PEK koji su sušeni pod ambijentalnim uslovima. Prinos, sadržaj ibuprofena, efikasnost inkorporiranja i sadržaj vlage PEK sušenih raspršivanjem bili su niži nego kod PEK sušenih pod ambijentalnim uslovima. Bolja protočnost PEK osušenih raspršivanjem je posledica skoro sfernog oblika čestica, što je pokazano skenirajućom elektronskom mikroskopijom. Rezultati DSC i PXRD analiza su potvrdili amorfizaciju ibuprofena tokom sušenja raspršivanjem. Ispitivani PEK osušeni pod različitim uslovima imali su visoku sposobnost rehidratacije u 0,1 M hlorovodoničnoj kiselini (pH 1,2) i fosfatnom puferu pH 7,4. In vitro oslobađanje ibuprofena iz osušenih PEK bilo je kontrolisano tokom 12 h uz oslobađanje približno 30% inkorporiranog ibuprofena. PEK sušeni raspršivanjem obezbedili su bolju kontrolu difuzije ibuprofena iz nosača u poređenju sa onima sušenim pod ambijentalnim uslovima.",
publisher = "Savez farmaceutskih udruženja Srbije",
journal = "Arhiv za farmaciju",
title = "Influence of spray-drying process on properties of chitosan/xanthan gum polyelectrolyte complexes as carriers for oral delivery of ibuprofen, Uticaj postupka sušenja raspršivanjem na svojstva polielektrolitnih kompleksa hitozana i ksantan gume kao nosača za peroralnu isporuku ibuprofena",
volume = "72",
number = "1",
pages = "36-60",
doi = "10.5937/arhfarm72-35133"
}

Ćirić, A., Milinković Budinčić, J., Medarević, Đ., Dobričić, V., Rmandić, M., Barudžija, T., Malenović, A., Petrović, L.,& Đekić, L.. (2022). Influence of spray-drying process on properties of chitosan/xanthan gum polyelectrolyte complexes as carriers for oral delivery of ibuprofen. in Arhiv za farmaciju
Savez farmaceutskih udruženja Srbije., 72(1), 36-60.
https://doi.org/10.5937/arhfarm72-35133

Ćirić A, Milinković Budinčić J, Medarević Đ, Dobričić V, Rmandić M, Barudžija T, Malenović A, Petrović L, Đekić L. Influence of spray-drying process on properties of chitosan/xanthan gum polyelectrolyte complexes as carriers for oral delivery of ibuprofen. in Arhiv za farmaciju. 2022;72(1):36-60.
doi:10.5937/arhfarm72-35133 .

Ćirić, Ana, Milinković Budinčić, Jelena, Medarević, Đorđe, Dobričić, Vladimir, Rmandić, Milena, Barudžija, Tanja, Malenović, Anđelija, Petrović, Lidija, Đekić, Ljiljana, "Influence of spray-drying process on properties of chitosan/xanthan gum polyelectrolyte complexes as carriers for oral delivery of ibuprofen" in Arhiv za farmaciju, 72, no. 1 (2022):36-60,
https://doi.org/10.5937/arhfarm72-35133 . .

TY  - CONF
AU  - Adamov, Ivana
AU  - Živanović, Jovana
AU  - Verovski, Ivana
AU  - Arsović, Natalija
AU  - Pešić, Nikola
AU  - Medarević, Đorđe
AU  - Grujić, Branka
AU  - Ibrić, Svetlana
PY  - 2022
UR  - https://farfar.pharmacy.bg.ac.rs/handle/123456789/5323
AB  - Introduction Three-dimensional (3D) printing as an innovative technology in the field of drug manufacturing has attracted a lot of attention from the scientific and professional public in recent years. Classified into seven main categories, all 3D printing techniques are based on the same layer-by-layer printing mechanism, where the structure of an object is created from a digital 3D file
using computer-aided design (CAD) software or imaging techniques (Trenfield et al., 2018). 3D printing techniques have the potential to provide
drug dosage forms of precise geometry and variety of shapes, with tendency to revolutionize the way drugs are designed and manufactured (Trenfield et al., 2018). 3D printing also pretends to play an important role in the concept of personalized medicine, allowing dose
adjustment according to individual patient needs based on their own characteristics, requirements and conditions of the disease, in order to achieve the most suitable
therapeutic outcomes. The approach of "one size fits all" could be changed by using 3D printing techniques in the manufacturing of small batches of patient-tailored medicines (Zema et al., 2017). In this study, digital light processing (DLP), also known as photopolymerization technique which utilizes light irradiation to create solid objects from photoreactive liquid resin, was used to fabricate fun-shaped oral dosage forms with an aim to achieve flexible dose adjustment of atomoxetine hydrochloride (AH), according to the specific needs of pediatric patients.
Materials and methods Materials Poly(ethylene glycol)diacrylate (PEGDA, average MW 250) was obtained from Sigma-Aldrich, Japan. Poly(ethylene glycol) (PEG 400, average MW 400) was purchased from Fagron B.V., The Netherlands. Mannitol Parteck® M 200 was obtained from Merck, Germany. AH
was kindly donated by Hemofarm AD, Vrsac, Serbia. Diphenyl(2,4,6-trimethylbenzoyl)phosphineoxide (DPPO) was purchased from Sigma-Aldrich, Germany. Preparation of photoreactive suspensions and 3D printing process Content of AH was 5% (w/w, formulation F1) or 10% (w/w, formulation F2). PEGDA and PEG 400 were used in a constant ratio of 3:1. Both formulations contained 0.50% of mannitol and 0.10% of DPPO. The water content was 5% (w/w, F1) or 10% (w/w, F2), depending on the amount of the active substance. Fun-shaped 3D models (Mickey Mouse, Ring, Pentagon and Cylinder) were designed in Autodesk fusion software version 2.0.8809 (Autodesk Inc, USA), exported as a stereolithography file (.stl) into the 3D printer software (Chitubox, version 1.7.0) and printed with Wanhao Duplicator 8 printer (Wanhao, China). 3D
models of Mickey Mouse and Ring were printed from formulation F1, while 3D models of Pentagon and Cylinder were printed from formulation F2.
Mass, dimensions and drug content determination 3D-printed dosage forms (n = 10) were weighed on an analytical balance (Kern & Sohn, Germany) and measured (length/diameter and thickness) using a digital caliper (Vogel Germany GmbH & Co. KG, Kevelaer, Germany). The drug content was determined UV spectrophotometrically (Evolution 300, Thermo Fisher Scientific, USA) at the wavelength of 270 nm. For standard preparation, 10 mg of AH was dissolved in 10 mL of absolute ethanol, shaken in an ultrasonic bath for 60 min at room temperature, cooled and then filtered through 0.45 μm filters (Millipore, USA). For test preparation one dosage form of each formulation was crushed and all samples underwent the same procedure as
described for standard preparation. In vitro drug release testing The dissolution test was performed with a USP-I Erweka DT 600 (Erweka, Germany) apparatus, in 500 mL of distilled water at 37 ± 0.5 °C, until a plateau was reached. The basket speed was fixed at 100 rpm, aliquots (5 mL) were withdrawn at time intervals of 15, 30, 45, 60, 120, 180, 240, 300, 360 and 420 min, respectively,
filtered through 0.45 μm filters and the amount of AH released was determined at 270 nm. Measurements were
performed in triplicate, for each formulation and each dosage form.
Differential Scanning Calorimetry (DSC) and Polarized Light Microscopy DSC was performed on a DSC 1 instrument (Mettler Toledo, Germany). Samples were subjected to heating at 10 °C/min in the range from 0 to 200 °C under constant nitrogen gas flow of 50 mL/min. The obtained data were
analyzed in the STARe software (version 12.10, Mettler, Toledo). An Olympus BX53-P polarized microscope
(Olympus, Japan) was used for visual examination of the internal structure, as well as for crystal detection. Photos were acquired using cellSens Entry Version 1.14 software (Olympus, Japan). Results and discussion Fun-shaped 3D models were successfully printed and printing time mainly depended on the geometry of the defined 3D model (on average, 10 minutes for 6 dosage forms), confirming the suitability of DLP technique for obtaining drugs of various shapes and sizes in a short period of time (Stanojević et al., 2021). All of the fabricated dosage forms had a smooth surface and a uniform shape. The dimensions and mass of the printed dosage forms varied to some extent, which was expected due to the phenomenon of light scattering caused by suspended drug particles (Stanojević et al., 2021). The
drug content depended on the amount of AH in the initial formulation and the geometry of the 3D model - 3.19 mg (Cylinder, F2), 4.42 mg (Ring, F1), 8.31 mg (Mickey Mouse, F1) and 26.51 mg (Pentagon, F2), respectively, which indicates the potential of the DLP technique to provide dosage forms with the possibility of "dose
tailoring" and individualization of therapy. The results of the dissolution test showed a prolonged release of AH from printed dosage forms. The Ring model exhibited the highest dissolution rate, which was consistent with its high surface area-to-volume ratio, while the Pentagon model exhibited the slowest drug release. DSC analysis showed broad endotherms between 60 and 80 °C, and the absence of sharp melting peak of AH. The drug crystals might have been dissolved during the heating process and therefore, samples were further analyzed by polarized light microscopy. Cross-sections indicated the presence of AH crystals, before and after the dissolution test, due to incomplete drug release from polymeric matrix. The layered structure was also observed confirming the fact that dosage forms were printed in a layer-by-layer
manner.
Conclusion Fun-shaped oral dosage forms with AH were successfully printed with DLP 3D printer. DLP 3D printing technique offers simple and fast way to fabricate innovative drug dosage forms, enabling flexible dose adjustments by varying the amount of incorporated active substance and the geometric shape of the created 3D
models, as well.
PB  - Macedonian Pharmaceutical Association
PB  - Faculty of Pharmacy, Ss Cyril and Methodius University in Skopje
C3  - Macedonian Pharmaceutical Bulletin
T1  - Fun-shaped oral dosage forms for the pediatric population fabricated by digital light processing (DLP) 3D printing technique
VL  - 68
IS  - Suppl 1
SP  - 293
EP  - 294
DO  - 10.33320/maced.pharm.bull.2022.68.03.141
ER  - 

@conference{
author = "Adamov, Ivana and Živanović, Jovana and Verovski, Ivana and Arsović, Natalija and Pešić, Nikola and Medarević, Đorđe and Grujić, Branka and Ibrić, Svetlana",
year = "2022",
abstract = "Introduction Three-dimensional (3D) printing as an innovative technology in the field of drug manufacturing has attracted a lot of attention from the scientific and professional public in recent years. Classified into seven main categories, all 3D printing techniques are based on the same layer-by-layer printing mechanism, where the structure of an object is created from a digital 3D file
using computer-aided design (CAD) software or imaging techniques (Trenfield et al., 2018). 3D printing techniques have the potential to provide
drug dosage forms of precise geometry and variety of shapes, with tendency to revolutionize the way drugs are designed and manufactured (Trenfield et al., 2018). 3D printing also pretends to play an important role in the concept of personalized medicine, allowing dose
adjustment according to individual patient needs based on their own characteristics, requirements and conditions of the disease, in order to achieve the most suitable
therapeutic outcomes. The approach of "one size fits all" could be changed by using 3D printing techniques in the manufacturing of small batches of patient-tailored medicines (Zema et al., 2017). In this study, digital light processing (DLP), also known as photopolymerization technique which utilizes light irradiation to create solid objects from photoreactive liquid resin, was used to fabricate fun-shaped oral dosage forms with an aim to achieve flexible dose adjustment of atomoxetine hydrochloride (AH), according to the specific needs of pediatric patients.
Materials and methods Materials Poly(ethylene glycol)diacrylate (PEGDA, average MW 250) was obtained from Sigma-Aldrich, Japan. Poly(ethylene glycol) (PEG 400, average MW 400) was purchased from Fagron B.V., The Netherlands. Mannitol Parteck® M 200 was obtained from Merck, Germany. AH
was kindly donated by Hemofarm AD, Vrsac, Serbia. Diphenyl(2,4,6-trimethylbenzoyl)phosphineoxide (DPPO) was purchased from Sigma-Aldrich, Germany. Preparation of photoreactive suspensions and 3D printing process Content of AH was 5% (w/w, formulation F1) or 10% (w/w, formulation F2). PEGDA and PEG 400 were used in a constant ratio of 3:1. Both formulations contained 0.50% of mannitol and 0.10% of DPPO. The water content was 5% (w/w, F1) or 10% (w/w, F2), depending on the amount of the active substance. Fun-shaped 3D models (Mickey Mouse, Ring, Pentagon and Cylinder) were designed in Autodesk fusion software version 2.0.8809 (Autodesk Inc, USA), exported as a stereolithography file (.stl) into the 3D printer software (Chitubox, version 1.7.0) and printed with Wanhao Duplicator 8 printer (Wanhao, China). 3D
models of Mickey Mouse and Ring were printed from formulation F1, while 3D models of Pentagon and Cylinder were printed from formulation F2.
Mass, dimensions and drug content determination 3D-printed dosage forms (n = 10) were weighed on an analytical balance (Kern & Sohn, Germany) and measured (length/diameter and thickness) using a digital caliper (Vogel Germany GmbH & Co. KG, Kevelaer, Germany). The drug content was determined UV spectrophotometrically (Evolution 300, Thermo Fisher Scientific, USA) at the wavelength of 270 nm. For standard preparation, 10 mg of AH was dissolved in 10 mL of absolute ethanol, shaken in an ultrasonic bath for 60 min at room temperature, cooled and then filtered through 0.45 μm filters (Millipore, USA). For test preparation one dosage form of each formulation was crushed and all samples underwent the same procedure as
described for standard preparation. In vitro drug release testing The dissolution test was performed with a USP-I Erweka DT 600 (Erweka, Germany) apparatus, in 500 mL of distilled water at 37 ± 0.5 °C, until a plateau was reached. The basket speed was fixed at 100 rpm, aliquots (5 mL) were withdrawn at time intervals of 15, 30, 45, 60, 120, 180, 240, 300, 360 and 420 min, respectively,
filtered through 0.45 μm filters and the amount of AH released was determined at 270 nm. Measurements were
performed in triplicate, for each formulation and each dosage form.
Differential Scanning Calorimetry (DSC) and Polarized Light Microscopy DSC was performed on a DSC 1 instrument (Mettler Toledo, Germany). Samples were subjected to heating at 10 °C/min in the range from 0 to 200 °C under constant nitrogen gas flow of 50 mL/min. The obtained data were
analyzed in the STARe software (version 12.10, Mettler, Toledo). An Olympus BX53-P polarized microscope
(Olympus, Japan) was used for visual examination of the internal structure, as well as for crystal detection. Photos were acquired using cellSens Entry Version 1.14 software (Olympus, Japan). Results and discussion Fun-shaped 3D models were successfully printed and printing time mainly depended on the geometry of the defined 3D model (on average, 10 minutes for 6 dosage forms), confirming the suitability of DLP technique for obtaining drugs of various shapes and sizes in a short period of time (Stanojević et al., 2021). All of the fabricated dosage forms had a smooth surface and a uniform shape. The dimensions and mass of the printed dosage forms varied to some extent, which was expected due to the phenomenon of light scattering caused by suspended drug particles (Stanojević et al., 2021). The
drug content depended on the amount of AH in the initial formulation and the geometry of the 3D model - 3.19 mg (Cylinder, F2), 4.42 mg (Ring, F1), 8.31 mg (Mickey Mouse, F1) and 26.51 mg (Pentagon, F2), respectively, which indicates the potential of the DLP technique to provide dosage forms with the possibility of "dose
tailoring" and individualization of therapy. The results of the dissolution test showed a prolonged release of AH from printed dosage forms. The Ring model exhibited the highest dissolution rate, which was consistent with its high surface area-to-volume ratio, while the Pentagon model exhibited the slowest drug release. DSC analysis showed broad endotherms between 60 and 80 °C, and the absence of sharp melting peak of AH. The drug crystals might have been dissolved during the heating process and therefore, samples were further analyzed by polarized light microscopy. Cross-sections indicated the presence of AH crystals, before and after the dissolution test, due to incomplete drug release from polymeric matrix. The layered structure was also observed confirming the fact that dosage forms were printed in a layer-by-layer
manner.
Conclusion Fun-shaped oral dosage forms with AH were successfully printed with DLP 3D printer. DLP 3D printing technique offers simple and fast way to fabricate innovative drug dosage forms, enabling flexible dose adjustments by varying the amount of incorporated active substance and the geometric shape of the created 3D
models, as well.",
publisher = "Macedonian Pharmaceutical Association, Faculty of Pharmacy, Ss Cyril and Methodius University in Skopje",
journal = "Macedonian Pharmaceutical Bulletin",
title = "Fun-shaped oral dosage forms for the pediatric population fabricated by digital light processing (DLP) 3D printing technique",
volume = "68",
number = "Suppl 1",
pages = "293-294",
doi = "10.33320/maced.pharm.bull.2022.68.03.141"
}

Adamov, I., Živanović, J., Verovski, I., Arsović, N., Pešić, N., Medarević, Đ., Grujić, B.,& Ibrić, S.. (2022). Fun-shaped oral dosage forms for the pediatric population fabricated by digital light processing (DLP) 3D printing technique. in Macedonian Pharmaceutical Bulletin
Macedonian Pharmaceutical Association., 68(Suppl 1), 293-294.
https://doi.org/10.33320/maced.pharm.bull.2022.68.03.141

Adamov I, Živanović J, Verovski I, Arsović N, Pešić N, Medarević Đ, Grujić B, Ibrić S. Fun-shaped oral dosage forms for the pediatric population fabricated by digital light processing (DLP) 3D printing technique. in Macedonian Pharmaceutical Bulletin. 2022;68(Suppl 1):293-294.
doi:10.33320/maced.pharm.bull.2022.68.03.141 .

Adamov, Ivana, Živanović, Jovana, Verovski, Ivana, Arsović, Natalija, Pešić, Nikola, Medarević, Đorđe, Grujić, Branka, Ibrić, Svetlana, "Fun-shaped oral dosage forms for the pediatric population fabricated by digital light processing (DLP) 3D printing technique" in Macedonian Pharmaceutical Bulletin, 68, no. Suppl 1 (2022):293-294,
https://doi.org/10.33320/maced.pharm.bull.2022.68.03.141 . .

TY  - CONF
AU  - Grujić, Branka
AU  - Jelić, Vesna
AU  - Medarević, Đorđe
PY  - 2022
UR  - https://farfar.pharmacy.bg.ac.rs/handle/123456789/5324
AB  - Introduction The study examined the development of barium sulphate tablets that do not dissolve in the digestive tract
and are used as a contrasting agent for measuring transit time through the column. The main problem for obtaining non-degradable tablets is the formation of a compact
polymer matrix that does not disintegrate in digestive fluids over a long period of time (Chaussade et al., 1986; Felder et al., 1984). In pharmaceutical technology, thermal techniques of granulation, extrusion, and the like, polymers and active pharmaceutical ingredients (APIs)
are known for achieving better solubility of low soluble substances or for achieving slow release of highly soluble substances from solid preparations (Obradović et al., 2016) Several different formulations were tested in which they were varied: the presence of different polymers Eudragit® RS PO and/or PMMA, wet granulation and direct compression procedure, different granulation of filler calcium hydrogen phosphate dihydrate, and the time of sintering in a pair of organic solvents of acetone or IPA at different time intervals. The results of the tensile
strength of the tablets that are important for the further sintering process and the degradability of sintered tablets were monitored as the output parameter. In the final
manufacturing process - tablet sintering, only formulations in which the tensile strength of the tablet was ≥20 MPa were used. For this reason, direct
compression tablets, as well as wet granulation formulations with PMMA, are not sintered. The tensile strength of the tablet before and after sintering indicates that the "wet" granulation is more efficient with IPA
because it produces better compacted granules (higher tensile strengths), while acetone is more efficient in the sintering process at 35oC , which is expected due to the higher vapor pressure at that temperature compared to the IPA.
Materials and Methods The tablets are made by the wet granulation process, and the direct compression process, and the pharmaceutical and technological characteristics of the tablets have been compared. The API Barium sulphate (Merck, Germany) was used. The essence of the formulation is based on the use of two polymers: polymethyl methacrylate (PMMA DP 300 U) and copolymers of ammonium methacrylic acid (Eudragit® RS PO).The role of PMMA DP 300 U is to with Eudragit® RS PO synergistically form in physiological
media an insoluble, completely impermeable and non-
swelling martix regardless of the pH value of the media.
Calcium hydrogen phosphate dihydrate, an insoluble excipient, was selected as the filler. Two types of this filler were selected, powder and fine granular (Emcompress®) intended for direct compression due to improved flowing and compressible properties. Magnesium stearate was used in order to achieve adequate lubrication and to eject the tablets from the matrix. Acetone and/or IPA were chosen as solvents in combination with concentrated ethanol and water. Wet granulation In laboratory tests, mixing and wet granulation were
carried out in a high shear mixer and dried at 50 °C in a fluidization oven. A vacuum processor was used for the pilot test. In the vacuum processor homogeneous mixing of the previously measured barium sulphate, calcium hydrogen phosphate dihydrate, Eudragit RS PO, and PMMA DP 300 U. The granulation solution is a mixture
of acetone or isopropanol, concentrated ethanol, and purified water, i.e. isopropanol and purified water and purified water. The wet agglomerated mass is dried in a vacuum processor by heating to a temperature of 50 °C.,
and the vacuum is included with occasional stirring until is achieved loss on drying of not more than 1% (at 105
oC). Magnesium stearate was added to the diluted granulate and further stirred. Tableting Compression of laboratory trials was performed on an eccentric tablet press EKO type, and pilot trials were performed on a Kilian rotary tablet press Synthesis 500.
For the 80 mg dose, the characteristics of the tablets were:
mass: 0.268 g, diameter: 8.8 - 9.2 mm, and hardness: at
least 20.0 MPa. Sintering Tablets were sintered in a sealed chamber saturated with either acetone vapor or isopropanol vapor at 35ºC (± 2 ºC) for 8h, 16h, 24h, 32h, and 40h. Drying After sintering, the tablets were dried or residual
acetone or isopropanol is removed to a maximum of 2.5 mg/tablet. The sintered tablets were dried according to the scheme: 1) Temperatures 22 ºC for 16 h, 2) 40ºC for 24 h, 3) 50 ºC for 8 h and 4) 55ºC for 8 h.
Results and discussion In the case of tablets made by direct compression, it
was not possible to achieve the corresponding mechanical characteristics of the tablets: the strength and friability, which were necessary for the further process and manipulation, or consolidation, by sintering in an organic solvent vapor. Formulation made with PMMA DP 300 U, without the addition of the Eudragit® RS PO polymer, could not be compressed due to the spherical shape of PMMA DP 300 U which is extremely unfavorable for compression. The results of tablet tensile strengths before
and after sintering indicate, for IPA and acetone solvents, that IPA solvent is more effective for wet granulation because it produces better compacting granules (higher tensile strengths are obtained), while acetone is in the sintering process at 35 °C a more efficient solvent, as expected given the higher vapor pressure at that temperature compared to IPA. The time interval during
which the disintegration was tested was up to 7 days because it is the interval during which the transit of the tablet through the column in subjects with slow passage is examined in vivo. When it comes to the efficiency of the
organic solvent in the process of polymer matrix consolidation by sintering, the slightly lower efficiency of isopropanol compared to acetone is observed. The
sintering time has a significantly greater effect on matrix consolidation. The criteria for intact barium sulphate tablets within a 7-day time interval was fulfilled only by formulations with a mixture of Eudragit® RS PO and PMMA DP 300 U polymers obtained by granulation with acetone or isopropanol using a sintered process during 35h. Conclusion Tests of various formulations and technological parameters in the production process have shown that in order to obtain a contrast agent for testing the functional radiology of the colon, rectum and anal canal, i.e. measuring the transit time through the colon, which meets the defined criteria, optimal formulation is with calcium hydrogen phosphate dihydrate powder, an equivalent amount of Eudragit RS PO and PMMA DP 300 U
polymers, isopropanol as solvent in addition to ethanol
and water in the process of wet granulation, and sintering process in an organic acetone solvent vapor at 35°C.
PB  - Macedonian Pharmaceutical Association
PB  - Faculty of Pharmacy, Ss Cyril and Methodius University in Skopje
C3  - Macedonian Pharmaceutical Bulletin
T1  - Pharmaceutical and technological characteristics of barium sulphate tablets -the screening of various formulation factors
VL  - 68
IS  - Suppl 1
SP  - 243
EP  - 244
DO  - 10.33320/maced.pharm.bull.2022.68.03.116
ER  - 

@conference{
author = "Grujić, Branka and Jelić, Vesna and Medarević, Đorđe",
year = "2022",
abstract = "Introduction The study examined the development of barium sulphate tablets that do not dissolve in the digestive tract
and are used as a contrasting agent for measuring transit time through the column. The main problem for obtaining non-degradable tablets is the formation of a compact
polymer matrix that does not disintegrate in digestive fluids over a long period of time (Chaussade et al., 1986; Felder et al., 1984). In pharmaceutical technology, thermal techniques of granulation, extrusion, and the like, polymers and active pharmaceutical ingredients (APIs)
are known for achieving better solubility of low soluble substances or for achieving slow release of highly soluble substances from solid preparations (Obradović et al., 2016) Several different formulations were tested in which they were varied: the presence of different polymers Eudragit® RS PO and/or PMMA, wet granulation and direct compression procedure, different granulation of filler calcium hydrogen phosphate dihydrate, and the time of sintering in a pair of organic solvents of acetone or IPA at different time intervals. The results of the tensile
strength of the tablets that are important for the further sintering process and the degradability of sintered tablets were monitored as the output parameter. In the final
manufacturing process - tablet sintering, only formulations in which the tensile strength of the tablet was ≥20 MPa were used. For this reason, direct
compression tablets, as well as wet granulation formulations with PMMA, are not sintered. The tensile strength of the tablet before and after sintering indicates that the "wet" granulation is more efficient with IPA
because it produces better compacted granules (higher tensile strengths), while acetone is more efficient in the sintering process at 35oC , which is expected due to the higher vapor pressure at that temperature compared to the IPA.
Materials and Methods The tablets are made by the wet granulation process, and the direct compression process, and the pharmaceutical and technological characteristics of the tablets have been compared. The API Barium sulphate (Merck, Germany) was used. The essence of the formulation is based on the use of two polymers: polymethyl methacrylate (PMMA DP 300 U) and copolymers of ammonium methacrylic acid (Eudragit® RS PO).The role of PMMA DP 300 U is to with Eudragit® RS PO synergistically form in physiological
media an insoluble, completely impermeable and non-
swelling martix regardless of the pH value of the media.
Calcium hydrogen phosphate dihydrate, an insoluble excipient, was selected as the filler. Two types of this filler were selected, powder and fine granular (Emcompress®) intended for direct compression due to improved flowing and compressible properties. Magnesium stearate was used in order to achieve adequate lubrication and to eject the tablets from the matrix. Acetone and/or IPA were chosen as solvents in combination with concentrated ethanol and water. Wet granulation In laboratory tests, mixing and wet granulation were
carried out in a high shear mixer and dried at 50 °C in a fluidization oven. A vacuum processor was used for the pilot test. In the vacuum processor homogeneous mixing of the previously measured barium sulphate, calcium hydrogen phosphate dihydrate, Eudragit RS PO, and PMMA DP 300 U. The granulation solution is a mixture
of acetone or isopropanol, concentrated ethanol, and purified water, i.e. isopropanol and purified water and purified water. The wet agglomerated mass is dried in a vacuum processor by heating to a temperature of 50 °C.,
and the vacuum is included with occasional stirring until is achieved loss on drying of not more than 1% (at 105
oC). Magnesium stearate was added to the diluted granulate and further stirred. Tableting Compression of laboratory trials was performed on an eccentric tablet press EKO type, and pilot trials were performed on a Kilian rotary tablet press Synthesis 500.
For the 80 mg dose, the characteristics of the tablets were:
mass: 0.268 g, diameter: 8.8 - 9.2 mm, and hardness: at
least 20.0 MPa. Sintering Tablets were sintered in a sealed chamber saturated with either acetone vapor or isopropanol vapor at 35ºC (± 2 ºC) for 8h, 16h, 24h, 32h, and 40h. Drying After sintering, the tablets were dried or residual
acetone or isopropanol is removed to a maximum of 2.5 mg/tablet. The sintered tablets were dried according to the scheme: 1) Temperatures 22 ºC for 16 h, 2) 40ºC for 24 h, 3) 50 ºC for 8 h and 4) 55ºC for 8 h.
Results and discussion In the case of tablets made by direct compression, it
was not possible to achieve the corresponding mechanical characteristics of the tablets: the strength and friability, which were necessary for the further process and manipulation, or consolidation, by sintering in an organic solvent vapor. Formulation made with PMMA DP 300 U, without the addition of the Eudragit® RS PO polymer, could not be compressed due to the spherical shape of PMMA DP 300 U which is extremely unfavorable for compression. The results of tablet tensile strengths before
and after sintering indicate, for IPA and acetone solvents, that IPA solvent is more effective for wet granulation because it produces better compacting granules (higher tensile strengths are obtained), while acetone is in the sintering process at 35 °C a more efficient solvent, as expected given the higher vapor pressure at that temperature compared to IPA. The time interval during
which the disintegration was tested was up to 7 days because it is the interval during which the transit of the tablet through the column in subjects with slow passage is examined in vivo. When it comes to the efficiency of the
organic solvent in the process of polymer matrix consolidation by sintering, the slightly lower efficiency of isopropanol compared to acetone is observed. The
sintering time has a significantly greater effect on matrix consolidation. The criteria for intact barium sulphate tablets within a 7-day time interval was fulfilled only by formulations with a mixture of Eudragit® RS PO and PMMA DP 300 U polymers obtained by granulation with acetone or isopropanol using a sintered process during 35h. Conclusion Tests of various formulations and technological parameters in the production process have shown that in order to obtain a contrast agent for testing the functional radiology of the colon, rectum and anal canal, i.e. measuring the transit time through the colon, which meets the defined criteria, optimal formulation is with calcium hydrogen phosphate dihydrate powder, an equivalent amount of Eudragit RS PO and PMMA DP 300 U
polymers, isopropanol as solvent in addition to ethanol
and water in the process of wet granulation, and sintering process in an organic acetone solvent vapor at 35°C.",
publisher = "Macedonian Pharmaceutical Association, Faculty of Pharmacy, Ss Cyril and Methodius University in Skopje",
journal = "Macedonian Pharmaceutical Bulletin",
title = "Pharmaceutical and technological characteristics of barium sulphate tablets -the screening of various formulation factors",
volume = "68",
number = "Suppl 1",
pages = "243-244",
doi = "10.33320/maced.pharm.bull.2022.68.03.116"
}

Grujić, B., Jelić, V.,& Medarević, Đ.. (2022). Pharmaceutical and technological characteristics of barium sulphate tablets -the screening of various formulation factors. in Macedonian Pharmaceutical Bulletin
Macedonian Pharmaceutical Association., 68(Suppl 1), 243-244.
https://doi.org/10.33320/maced.pharm.bull.2022.68.03.116

Grujić B, Jelić V, Medarević Đ. Pharmaceutical and technological characteristics of barium sulphate tablets -the screening of various formulation factors. in Macedonian Pharmaceutical Bulletin. 2022;68(Suppl 1):243-244.
doi:10.33320/maced.pharm.bull.2022.68.03.116 .

Grujić, Branka, Jelić, Vesna, Medarević, Đorđe, "Pharmaceutical and technological characteristics of barium sulphate tablets -the screening of various formulation factors" in Macedonian Pharmaceutical Bulletin, 68, no. Suppl 1 (2022):243-244,
https://doi.org/10.33320/maced.pharm.bull.2022.68.03.116 . .

TY  - CONF
AU  - Pešić, Nikola
AU  - Krkobabić, Mirjana
AU  - Adamov, Ivana
AU  - Ibrić, Svetlana
AU  - Ivković, Branka
AU  - Medarević, Đorđe
PY  - 2022
UR  - https://farfar.pharmacy.bg.ac.rs/handle/123456789/4749
AB  - 1. INTRODUCTION
When it comes to pharmacy, 3D printing has
gained immense popularity in recent years due
to its revolutionary use in printing drugs tailored
to individual patient needs [1,2]. Selective laser
sintering (SLS) is an industrial 3D printing
technique which uses a powder bed to build up
the 3D object thanks to a laser which binds the
powder particles together. Advantages of SLS
technique include the fact that it is a solvent-free
process and offers relatively fast production.
Until today, a limited number of studies
investigating the production of drug dosage
forms using SLS have been reported [2,3].
2. MATERIALS AND METHODS
2.1. Materials
Carvedilol (CRV) was used as a model
substance in this study and it was donated by
Hemofarm (Vršac, Serbia). The following
excipients used to obtain 3D printing tablets:
polyvinyl alcohol (PVA, Merck), mannitol
(Parteck® M, Merck), Ludipress®
(coprocessed excipient consisting of 93%
lactose monohydrate, 3.5% crospovidone
(Kollidon® CL) and 3.5% povidone K30
(Kollidon® 30), BASF), talc (Merck) and
candurin (Candurin® Gold Sheen, Merck).
2.2. Preparation of formulations
The compositions of the formulations are
shown in Table 1.
Table 1. Composition of the formulations
Material Formulation 1 Formulation 2
CRV 10% 10%
PVA 55% 55%
Parteck® M 30% /
Ludipress® / 30%
Talc 2% 2%
Candurin®
Gold Sheen 3% 3%
Powder for 3D printing was obtained by mixing
all the components of the formulation and
sifting through a sieve with a diameter of 180
μm.
2.3. 3D printing of oral dosage forms
A cylindrical 3D models of the printed tablets
(8.00 mm diameter and 2.00 mm thickness)
were designed with Autodesk Fusion 360
software version 2.0.8809 (Autodesk Inc, San
Rafael, CA, USA), exported as a
stereolithography file (.stl) and printed with
Sintratec Kit 3D printer (Sintratec AG,
Switzerland). The printing parameters were
controlled using Sintratec 3D printer software.
After a series of variations in temperature and
laser speed, the optimal values of these
parameters used in the 3D printing process were
established and shown in Table 2.
Table 2. SLS 3D printing process parameters
Surface
Temperature
( ◦C)
Chamber
Temperature
( ◦C)
Laser
speed
(mm/s)
Hatch
space
80 ºC 70 ºC 60 250 μm
2.4. Mechanical properties of 3D tablets
Tablets (n = 10) were weighed on a Sartorius BP
210 D analytical balance (Sartorius, Goettingen,
Germany) and measured (diameter and
thickness) using a digital caliper (Vogel,
Kevelaer, Germany).
2.5. Powder X-ray diffraction analysis
(PXRD)
PXRD analysis was performed to assess
whether the laser induced amorphization of any
of the compounds, especially amorphization of
poorly soluble CRV. Samples were collected
using a Philips PW-1050 (Philips, The
Netherlands) diffractometer, operated at 40 kV
and 30 mA, using Ni-filtered Cu Kα radiation.
2.6. Dissolution and Drug Release Analysis
Dissolution testing was performed under nonsink
conditions using mini paddle apparatus
(Erweka DT 600, Germany) with a paddle
rotation speed of 50 rpm for 8 h, in 100 ml of
phosphate buffer (pH 6.8). The amount of
dissolved CRV was determined by HPLC
method using Dionex Ultimate 3000 (Thermo
Scientific, USA) HPLC system.
3. RESULTS AND DISCUSSION
3.1. 3D printing process
It was shown that SLS printer was able to
fabricate 3D tablets with CRV, as well as that
success of the printing process depended on the
used printing parameters.
3.2. Mechanical properties of 3D tablets
The dimensions of the obtained 3D tablets were
in accordance with the defined values of the
created 3D models (F1: 8.10 ± 0.08 mm
diameter and 2.10 ± 0.13 mm thickness, F2:
8.13 ± 0.09 mm diameter and 2.10 ± 0.12 mm
thickness). Significant variations in tablet
weight between formulations were not observed
(m1=0.146 ± 0.04; m2=0.136 ± 0.03).
3.3. Powder X-ray diffraction analysis
(PXRD)
Figure 1. The X-ray powder diffraction of F1
and F2.
3.4. Dissolution and Drug Release Analysis
Figure 2. Dissolution profiles of 3D printing
tablets
4. CONCLUSION
SLA represents a new chapter in 3D printing of
solid oral dosage forms and in individualized
therapy in particular. By adjusting the
formulation and process parameters, it was
possible to produce SLS tablets with coamorphous
CRV and PVA as a main polymer.
Complete drug release was achieved under non
sink conditions after 8 hours in phosphate
buffer. The tailoring of drug release might be
achieved by varying formulation factors as well
as process parameters, although it could be
governed by the composition of the whole
formulation.
PB  - Slovensko farmacevtsko društvo in Univerza v Ljubljani, Fakulteta za farmacijo
C3  - 9th BBBB International Conference on Pharmaceutical Sciences Pharma Sciences of Tomorrow: Book of Abstracts
T1  - Oral dosage forms with carvedilol fabricated by selective laser sintering (SLS) 3D printing technique
SP  - 210
EP  - 211
UR  - https://hdl.handle.net/21.15107/rcub_farfar_4749
ER  - 

@conference{
author = "Pešić, Nikola and Krkobabić, Mirjana and Adamov, Ivana and Ibrić, Svetlana and Ivković, Branka and Medarević, Đorđe",
year = "2022",
abstract = "1. INTRODUCTION
When it comes to pharmacy, 3D printing has
gained immense popularity in recent years due
to its revolutionary use in printing drugs tailored
to individual patient needs [1,2]. Selective laser
sintering (SLS) is an industrial 3D printing
technique which uses a powder bed to build up
the 3D object thanks to a laser which binds the
powder particles together. Advantages of SLS
technique include the fact that it is a solvent-free
process and offers relatively fast production.
Until today, a limited number of studies
investigating the production of drug dosage
forms using SLS have been reported [2,3].
2. MATERIALS AND METHODS
2.1. Materials
Carvedilol (CRV) was used as a model
substance in this study and it was donated by
Hemofarm (Vršac, Serbia). The following
excipients used to obtain 3D printing tablets:
polyvinyl alcohol (PVA, Merck), mannitol
(Parteck® M, Merck), Ludipress®
(coprocessed excipient consisting of 93%
lactose monohydrate, 3.5% crospovidone
(Kollidon® CL) and 3.5% povidone K30
(Kollidon® 30), BASF), talc (Merck) and
candurin (Candurin® Gold Sheen, Merck).
2.2. Preparation of formulations
The compositions of the formulations are
shown in Table 1.
Table 1. Composition of the formulations
Material Formulation 1 Formulation 2
CRV 10% 10%
PVA 55% 55%
Parteck® M 30% /
Ludipress® / 30%
Talc 2% 2%
Candurin®
Gold Sheen 3% 3%
Powder for 3D printing was obtained by mixing
all the components of the formulation and
sifting through a sieve with a diameter of 180
μm.
2.3. 3D printing of oral dosage forms
A cylindrical 3D models of the printed tablets
(8.00 mm diameter and 2.00 mm thickness)
were designed with Autodesk Fusion 360
software version 2.0.8809 (Autodesk Inc, San
Rafael, CA, USA), exported as a
stereolithography file (.stl) and printed with
Sintratec Kit 3D printer (Sintratec AG,
Switzerland). The printing parameters were
controlled using Sintratec 3D printer software.
After a series of variations in temperature and
laser speed, the optimal values of these
parameters used in the 3D printing process were
established and shown in Table 2.
Table 2. SLS 3D printing process parameters
Surface
Temperature
( ◦C)
Chamber
Temperature
( ◦C)
Laser
speed
(mm/s)
Hatch
space
80 ºC 70 ºC 60 250 μm
2.4. Mechanical properties of 3D tablets
Tablets (n = 10) were weighed on a Sartorius BP
210 D analytical balance (Sartorius, Goettingen,
Germany) and measured (diameter and
thickness) using a digital caliper (Vogel,
Kevelaer, Germany).
2.5. Powder X-ray diffraction analysis
(PXRD)
PXRD analysis was performed to assess
whether the laser induced amorphization of any
of the compounds, especially amorphization of
poorly soluble CRV. Samples were collected
using a Philips PW-1050 (Philips, The
Netherlands) diffractometer, operated at 40 kV
and 30 mA, using Ni-filtered Cu Kα radiation.
2.6. Dissolution and Drug Release Analysis
Dissolution testing was performed under nonsink
conditions using mini paddle apparatus
(Erweka DT 600, Germany) with a paddle
rotation speed of 50 rpm for 8 h, in 100 ml of
phosphate buffer (pH 6.8). The amount of
dissolved CRV was determined by HPLC
method using Dionex Ultimate 3000 (Thermo
Scientific, USA) HPLC system.
3. RESULTS AND DISCUSSION
3.1. 3D printing process
It was shown that SLS printer was able to
fabricate 3D tablets with CRV, as well as that
success of the printing process depended on the
used printing parameters.
3.2. Mechanical properties of 3D tablets
The dimensions of the obtained 3D tablets were
in accordance with the defined values of the
created 3D models (F1: 8.10 ± 0.08 mm
diameter and 2.10 ± 0.13 mm thickness, F2:
8.13 ± 0.09 mm diameter and 2.10 ± 0.12 mm
thickness). Significant variations in tablet
weight between formulations were not observed
(m1=0.146 ± 0.04; m2=0.136 ± 0.03).
3.3. Powder X-ray diffraction analysis
(PXRD)
Figure 1. The X-ray powder diffraction of F1
and F2.
3.4. Dissolution and Drug Release Analysis
Figure 2. Dissolution profiles of 3D printing
tablets
4. CONCLUSION
SLA represents a new chapter in 3D printing of
solid oral dosage forms and in individualized
therapy in particular. By adjusting the
formulation and process parameters, it was
possible to produce SLS tablets with coamorphous
CRV and PVA as a main polymer.
Complete drug release was achieved under non
sink conditions after 8 hours in phosphate
buffer. The tailoring of drug release might be
achieved by varying formulation factors as well
as process parameters, although it could be
governed by the composition of the whole
formulation.",
publisher = "Slovensko farmacevtsko društvo in Univerza v Ljubljani, Fakulteta za farmacijo",
journal = "9th BBBB International Conference on Pharmaceutical Sciences Pharma Sciences of Tomorrow: Book of Abstracts",
title = "Oral dosage forms with carvedilol fabricated by selective laser sintering (SLS) 3D printing technique",
pages = "210-211",
url = "https://hdl.handle.net/21.15107/rcub_farfar_4749"
}

Pešić, N., Krkobabić, M., Adamov, I., Ibrić, S., Ivković, B.,& Medarević, Đ.. (2022). Oral dosage forms with carvedilol fabricated by selective laser sintering (SLS) 3D printing technique. in 9th BBBB International Conference on Pharmaceutical Sciences Pharma Sciences of Tomorrow: Book of Abstracts
Slovensko farmacevtsko društvo in Univerza v Ljubljani, Fakulteta za farmacijo., 210-211.
https://hdl.handle.net/21.15107/rcub_farfar_4749

Pešić N, Krkobabić M, Adamov I, Ibrić S, Ivković B, Medarević Đ. Oral dosage forms with carvedilol fabricated by selective laser sintering (SLS) 3D printing technique. in 9th BBBB International Conference on Pharmaceutical Sciences Pharma Sciences of Tomorrow: Book of Abstracts. 2022;:210-211.
https://hdl.handle.net/21.15107/rcub_farfar_4749 .

Pešić, Nikola, Krkobabić, Mirjana, Adamov, Ivana, Ibrić, Svetlana, Ivković, Branka, Medarević, Đorđe, "Oral dosage forms with carvedilol fabricated by selective laser sintering (SLS) 3D printing technique" in 9th BBBB International Conference on Pharmaceutical Sciences Pharma Sciences of Tomorrow: Book of Abstracts (2022):210-211,
https://hdl.handle.net/21.15107/rcub_farfar_4749 .

TY  - CONF
AU  - Adamov, Ivana
AU  - Tenić, Milica
AU  - Pešić, Nikola
AU  - Medarević, Đorđe
AU  - Ivković, Branka
AU  - Ibrić, Svetlana
PY  - 2022
UR  - https://farfar.pharmacy.bg.ac.rs/handle/123456789/4573
AB  - In recent years, introduction of modern technologies, such as 3D printing, has
opened a new chapter and caused a paradigm shift from manufacturing of large-scale to
small batches of medicines tailored accordingly to the specific needs of patients (1). The aim
of this study was to formulate and fabricate two-layered tablets using digital light processing
(DLP) technique, which utilizes light irradiation to create solid objects from photoreactive
liquid resin in a layer-by-layer manner. Hydrochlorothiazide (HHT, 5%,w/w) and warfarin
sodium (VRN, 5%,w/w) were selected as model drugs, commonly used together in the
treatment of cardiovascular diseases. 3D printing process was initiated with 0.10% of
photoinitiator, at a constant ratio of poly(ethylene glycol)diacrylate and poly(ethylene
glycol) 400, 1:1, with the addition of water (10%,w/w). 3D tablets, with each of the active
substances in a separate layer, 8.00 mm in diameter and 1.50 mm thick, as well as combined
two-layered tablets with HHT and VRN in individual layers, were successfully printed with
Wanhao D8 printer. Dissolution test results showed immediate, but incomplete release of
VRN (81.47 ± 1.47%, after 45 min) from individual layers, while the release of HHT was
prolonged and complete (98.17 ± 3.11%, after 8 h). Significantly slower and incomplete
release of VRN and HHT from combined tablets was observed. The absence of interactions
and the presence of a layered structure were confirmed. DLP technique has a potential to
provide fast fabrication of combined tablets, while further optimization of formulation
factors is necessary in order to achieve complete drug release.
AB  - Poslednjih godina, uvođenjem savremenih tehnologija, poput 3D štampe, otvorilo se
novo poglavlje u načinu proizvodnje lekova i uslovilo razvoj fundamentalnih promena, pri
čemu serijska proizvodnja velikih šarži pretenduje da bude zamenjena malim serijama
lekova prilagođenih specifičnim potrebama pacijenata (1). Cilj ovog istraživanja bio je da se
formulišu i izrade dvoslojne tablete primenom tehnike digitalne obrade svetlosti (DLP) koja
omogućava dobijanje objekata mehanizmom nanošenja materijala “sloj po sloj” iz tečne
fotopolimerizacione smole pod uticajem svetlosti. Hidrohlortiazid (HHT, 5%, m/m) i
varfarin-natrijum (VRN, 5%, m/m) odabrani su kao model lekovite supstance, koje se obično
primenjuju zajedno u lečenju kardiovaskularnih bolesti. Proces 3D štampanja sproveden je u
prisustvu 0,10% fotoinicijatora, pri konstantnom masenom odnosu poli(etilen
glikol)diakrilata i poli(etilen glikola) 400, 1:1, uz dodatak 10% vode. 3D tablete, sa svakom
od aktivnih supstanci u posebnom sloju, prečnika 8,00 mm i debljine 1,50 mm, kao i
kombinovane dvoslojne tablete sa HHT i VRN u pojedinačnim slojevima, uspešno su
odštampane u Wanhao D8 štampaču. Prilikom ispitivanja brzine rastvaranja lekovite
supstance iz pojedinačnih slojeva, došlo je do trenutnog (81,47 ± 1,47% nakon 45 min), ali
nepotpunog oslobađanja VRN, dok je HHT u potpunosti oslobođen, prateći kinetiku
produženog oslobađanja (98,17 ± 3,11%, nakon 8 h). Zapaženo je znatno sporije i nepotpuno
oslobađanje VRN i HHT iz kombinovanih dvoslojnih tableta, nakon 8 h. Potvrđeno je
odsustvo interakcija i prisustvo slojevite strukture. DLP tehnika ima potencijal da obezbedi
brzu izradu kombinovanih tableta, pri čemu je neophodna dalja optimizacija formulacionih
faktora u cilju postizanja potpunog oslobađanja lekovite supstance.
PB  - Savez farmaceutskih udruženja Srbije (SFUS)
C3  - Arhiv za farmaciju
T1  - Application of 3D printing photopolymerization technique in the fabrication of two-layered tablets
T1  - Primena fotopolimerizacione tehnike 3D štampe lekova u izradi dvoslojnih tableta
VL  - 72
IS  - 4 suplement
SP  - S410
EP  - S411
UR  - https://hdl.handle.net/21.15107/rcub_farfar_4573
ER  - 

@conference{
author = "Adamov, Ivana and Tenić, Milica and Pešić, Nikola and Medarević, Đorđe and Ivković, Branka and Ibrić, Svetlana",
year = "2022",
abstract = "In recent years, introduction of modern technologies, such as 3D printing, has
opened a new chapter and caused a paradigm shift from manufacturing of large-scale to
small batches of medicines tailored accordingly to the specific needs of patients (1). The aim
of this study was to formulate and fabricate two-layered tablets using digital light processing
(DLP) technique, which utilizes light irradiation to create solid objects from photoreactive
liquid resin in a layer-by-layer manner. Hydrochlorothiazide (HHT, 5%,w/w) and warfarin
sodium (VRN, 5%,w/w) were selected as model drugs, commonly used together in the
treatment of cardiovascular diseases. 3D printing process was initiated with 0.10% of
photoinitiator, at a constant ratio of poly(ethylene glycol)diacrylate and poly(ethylene
glycol) 400, 1:1, with the addition of water (10%,w/w). 3D tablets, with each of the active
substances in a separate layer, 8.00 mm in diameter and 1.50 mm thick, as well as combined
two-layered tablets with HHT and VRN in individual layers, were successfully printed with
Wanhao D8 printer. Dissolution test results showed immediate, but incomplete release of
VRN (81.47 ± 1.47%, after 45 min) from individual layers, while the release of HHT was
prolonged and complete (98.17 ± 3.11%, after 8 h). Significantly slower and incomplete
release of VRN and HHT from combined tablets was observed. The absence of interactions
and the presence of a layered structure were confirmed. DLP technique has a potential to
provide fast fabrication of combined tablets, while further optimization of formulation
factors is necessary in order to achieve complete drug release., Poslednjih godina, uvođenjem savremenih tehnologija, poput 3D štampe, otvorilo se
novo poglavlje u načinu proizvodnje lekova i uslovilo razvoj fundamentalnih promena, pri
čemu serijska proizvodnja velikih šarži pretenduje da bude zamenjena malim serijama
lekova prilagođenih specifičnim potrebama pacijenata (1). Cilj ovog istraživanja bio je da se
formulišu i izrade dvoslojne tablete primenom tehnike digitalne obrade svetlosti (DLP) koja
omogućava dobijanje objekata mehanizmom nanošenja materijala “sloj po sloj” iz tečne
fotopolimerizacione smole pod uticajem svetlosti. Hidrohlortiazid (HHT, 5%, m/m) i
varfarin-natrijum (VRN, 5%, m/m) odabrani su kao model lekovite supstance, koje se obično
primenjuju zajedno u lečenju kardiovaskularnih bolesti. Proces 3D štampanja sproveden je u
prisustvu 0,10% fotoinicijatora, pri konstantnom masenom odnosu poli(etilen
glikol)diakrilata i poli(etilen glikola) 400, 1:1, uz dodatak 10% vode. 3D tablete, sa svakom
od aktivnih supstanci u posebnom sloju, prečnika 8,00 mm i debljine 1,50 mm, kao i
kombinovane dvoslojne tablete sa HHT i VRN u pojedinačnim slojevima, uspešno su
odštampane u Wanhao D8 štampaču. Prilikom ispitivanja brzine rastvaranja lekovite
supstance iz pojedinačnih slojeva, došlo je do trenutnog (81,47 ± 1,47% nakon 45 min), ali
nepotpunog oslobađanja VRN, dok je HHT u potpunosti oslobođen, prateći kinetiku
produženog oslobađanja (98,17 ± 3,11%, nakon 8 h). Zapaženo je znatno sporije i nepotpuno
oslobađanje VRN i HHT iz kombinovanih dvoslojnih tableta, nakon 8 h. Potvrđeno je
odsustvo interakcija i prisustvo slojevite strukture. DLP tehnika ima potencijal da obezbedi
brzu izradu kombinovanih tableta, pri čemu je neophodna dalja optimizacija formulacionih
faktora u cilju postizanja potpunog oslobađanja lekovite supstance.",
publisher = "Savez farmaceutskih udruženja Srbije (SFUS)",
journal = "Arhiv za farmaciju",
title = "Application of 3D printing photopolymerization technique in the fabrication of two-layered tablets, Primena fotopolimerizacione tehnike 3D štampe lekova u izradi dvoslojnih tableta",
volume = "72",
number = "4 suplement",
pages = "S410-S411",
url = "https://hdl.handle.net/21.15107/rcub_farfar_4573"
}

Adamov, I., Tenić, M., Pešić, N., Medarević, Đ., Ivković, B.,& Ibrić, S.. (2022). Application of 3D printing photopolymerization technique in the fabrication of two-layered tablets. in Arhiv za farmaciju
Savez farmaceutskih udruženja Srbije (SFUS)., 72(4 suplement), S410-S411.
https://hdl.handle.net/21.15107/rcub_farfar_4573

Adamov I, Tenić M, Pešić N, Medarević Đ, Ivković B, Ibrić S. Application of 3D printing photopolymerization technique in the fabrication of two-layered tablets. in Arhiv za farmaciju. 2022;72(4 suplement):S410-S411.
https://hdl.handle.net/21.15107/rcub_farfar_4573 .

Adamov, Ivana, Tenić, Milica, Pešić, Nikola, Medarević, Đorđe, Ivković, Branka, Ibrić, Svetlana, "Application of 3D printing photopolymerization technique in the fabrication of two-layered tablets" in Arhiv za farmaciju, 72, no. 4 suplement (2022):S410-S411,
https://hdl.handle.net/21.15107/rcub_farfar_4573 .

TY  - JOUR
AU  - Adamov, Ivana
AU  - Medarević, Đorđe
AU  - Ivković, Branka
AU  - Ivković, Aleksandar
AU  - Ibrić, Svetlana
PY  - 2022
UR  - https://farfar.pharmacy.bg.ac.rs/handle/123456789/4411
AB  - Ever since 3D printing was introduced to the field of pharmacy, it has caused a paradigm
shift from the manufacturing of large-scale to small batches of medicines tailored accordingly to
the specific needs of patients. This study aimed to formulate and fabricate two-layered 3D tablets
using the digital light processing (DLP) technique. Hydrochlorothiazide (HHT,5%,w/w) and
warfarin sodium (WS,5%,w/w) were selected as model drugs. The printing process was initiated
with 0.1% of photoinitiator, at a constant ratio of poly(ethylene glycol)diacrylate and
poly(ethylene glycol) 400, 1:1, with the addition of water (10%,w/w). Single-layered tablets of
8.00 mm diameter and 1.50 mm thickness, containing HHT and WS respectively, were
successfully printed, as well as combined two-layered 3D tablets, with each of the active
substances in separate layers. Dissolution tests of single-layered tablets showed immediate, but
incomplete release of WS (81.47±1.47%, after 45min), and prolonged and complete release of
HHT (98.17±3.11%, after 8h), while significantly slower and incomplete release of both drugs
from the combined two-layered 3D tablets was observed. The absence of drug-polymer
interaction and presence of a layered cross-sectional tablet structure were confirmed. DLP
technique enables simple and rapid fabrication of combined two-layered 3D tablets, while further
optimization of formulation factors is necessary to achieve complete drug release.
AB  - Uvođenje tehnologije 3D štampe u oblasti farmacije uslovilo je razvoj fundamentalnih promena, pri čemu serijska proizvodnja velikih šarži pretenduje da bude zamenjena malim serijama lekova prilagođenih prema specifičnim potrebama pacijenata. Cilj istraživanja bio je da se formulišu i izrade dvoslojne tablete primenom tehnike digitalne obrade svetlosti (DLP). Hidrohlortiazid (HHT, 5%, m/m) i varfarin-natrijum (WS, 5%, m/m) odabrani su kao model lekovite supstance. Proces štampanja sproveden je u prisustvu 0,1% fotoinicijatora, pri konstantnom masenom odnosu poli(etilen glikol)diakrilata i poli(etilen glikola) 400, 1:1, uz dodatak 10% vode. Jednoslojne 3D tablete prečnika 8,00 mm i debljine 1,50 mm, koje sadrže HHT, odnosno WS, kao i kombinovane dvoslojne 3D tablete, sa svakom od aktivnih supstanci u posebnom sloju, uspešno su odštampane. Prilikom ispitivanja brzine rastvaranja lekovite supstance iz jednoslojnih tableta, došlo je do trenutnog (81,47±1,47%, nakon 45 min), ali nepotpunog oslobađanja WS, i produženog i potpunog oslobađanja HHT (98,17±3,11%, nakon 8 h), dok je iz kombinovanih tableta zapaženo znatno sporije i nepotpuno oslobađanje obe lekovite supstance. Potvrđeno je odsustvo interakcija i prisustvo slojevite strukture. DLP tehnika pruža mogućnost jednostavne i brze izrade kombinovanih tableta, pri čemu je dalja optimizacija formulacionih faktora neophodna u cilju postizanja potpunog oslobađanja lekovite supstance.
PB  - Pharmaceutical Association of Serbia
T2  - Arhiv za farmaciju
T1  - Digital light processing (DLP) 3D printing technique applied in the fabrication of two-layered tablets: the concept of a combined polypill
T1  - 3D tehnika digitalne obrade svetlosti (DLP) primenjena u izradi dvoslojnih tableta: koncept kombinovane polipilule
VL  - 72
IS  - 6
SP  - 674
EP  - 688
DO  - 10.5937/arhfarm72-40365
ER  - 

@article{
author = "Adamov, Ivana and Medarević, Đorđe and Ivković, Branka and Ivković, Aleksandar and Ibrić, Svetlana",
year = "2022",
abstract = "Ever since 3D printing was introduced to the field of pharmacy, it has caused a paradigm
shift from the manufacturing of large-scale to small batches of medicines tailored accordingly to
the specific needs of patients. This study aimed to formulate and fabricate two-layered 3D tablets
using the digital light processing (DLP) technique. Hydrochlorothiazide (HHT,5%,w/w) and
warfarin sodium (WS,5%,w/w) were selected as model drugs. The printing process was initiated
with 0.1% of photoinitiator, at a constant ratio of poly(ethylene glycol)diacrylate and
poly(ethylene glycol) 400, 1:1, with the addition of water (10%,w/w). Single-layered tablets of
8.00 mm diameter and 1.50 mm thickness, containing HHT and WS respectively, were
successfully printed, as well as combined two-layered 3D tablets, with each of the active
substances in separate layers. Dissolution tests of single-layered tablets showed immediate, but
incomplete release of WS (81.47±1.47%, after 45min), and prolonged and complete release of
HHT (98.17±3.11%, after 8h), while significantly slower and incomplete release of both drugs
from the combined two-layered 3D tablets was observed. The absence of drug-polymer
interaction and presence of a layered cross-sectional tablet structure were confirmed. DLP
technique enables simple and rapid fabrication of combined two-layered 3D tablets, while further
optimization of formulation factors is necessary to achieve complete drug release., Uvođenje tehnologije 3D štampe u oblasti farmacije uslovilo je razvoj fundamentalnih promena, pri čemu serijska proizvodnja velikih šarži pretenduje da bude zamenjena malim serijama lekova prilagođenih prema specifičnim potrebama pacijenata. Cilj istraživanja bio je da se formulišu i izrade dvoslojne tablete primenom tehnike digitalne obrade svetlosti (DLP). Hidrohlortiazid (HHT, 5%, m/m) i varfarin-natrijum (WS, 5%, m/m) odabrani su kao model lekovite supstance. Proces štampanja sproveden je u prisustvu 0,1% fotoinicijatora, pri konstantnom masenom odnosu poli(etilen glikol)diakrilata i poli(etilen glikola) 400, 1:1, uz dodatak 10% vode. Jednoslojne 3D tablete prečnika 8,00 mm i debljine 1,50 mm, koje sadrže HHT, odnosno WS, kao i kombinovane dvoslojne 3D tablete, sa svakom od aktivnih supstanci u posebnom sloju, uspešno su odštampane. Prilikom ispitivanja brzine rastvaranja lekovite supstance iz jednoslojnih tableta, došlo je do trenutnog (81,47±1,47%, nakon 45 min), ali nepotpunog oslobađanja WS, i produženog i potpunog oslobađanja HHT (98,17±3,11%, nakon 8 h), dok je iz kombinovanih tableta zapaženo znatno sporije i nepotpuno oslobađanje obe lekovite supstance. Potvrđeno je odsustvo interakcija i prisustvo slojevite strukture. DLP tehnika pruža mogućnost jednostavne i brze izrade kombinovanih tableta, pri čemu je dalja optimizacija formulacionih faktora neophodna u cilju postizanja potpunog oslobađanja lekovite supstance.",
publisher = "Pharmaceutical Association of Serbia",
journal = "Arhiv za farmaciju",
title = "Digital light processing (DLP) 3D printing technique applied in the fabrication of two-layered tablets: the concept of a combined polypill, 3D tehnika digitalne obrade svetlosti (DLP) primenjena u izradi dvoslojnih tableta: koncept kombinovane polipilule",
volume = "72",
number = "6",
pages = "674-688",
doi = "10.5937/arhfarm72-40365"
}

Adamov, I., Medarević, Đ., Ivković, B., Ivković, A.,& Ibrić, S.. (2022). Digital light processing (DLP) 3D printing technique applied in the fabrication of two-layered tablets: the concept of a combined polypill. in Arhiv za farmaciju
Pharmaceutical Association of Serbia., 72(6), 674-688.
https://doi.org/10.5937/arhfarm72-40365

Adamov I, Medarević Đ, Ivković B, Ivković A, Ibrić S. Digital light processing (DLP) 3D printing technique applied in the fabrication of two-layered tablets: the concept of a combined polypill. in Arhiv za farmaciju. 2022;72(6):674-688.
doi:10.5937/arhfarm72-40365 .

Adamov, Ivana, Medarević, Đorđe, Ivković, Branka, Ivković, Aleksandar, Ibrić, Svetlana, "Digital light processing (DLP) 3D printing technique applied in the fabrication of two-layered tablets: the concept of a combined polypill" in Arhiv za farmaciju, 72, no. 6 (2022):674-688,
https://doi.org/10.5937/arhfarm72-40365 . .

TY  - JOUR
AU  - Adamov, Ivana
AU  - Stanojević, Gordana
AU  - Medarević, Đorđe
AU  - Ivković, Branka
AU  - Kočović, David
AU  - Mirković, Dušica
AU  - Ibrić, Svetlana
PY  - 2022
UR  - https://farfar.pharmacy.bg.ac.rs/handle/123456789/4275
AB  - The introduction of three-dimensional (3D) printing in the pharmaceutical field has made great strides towards innovations in the way drugs are designed and manufactured. In this study, digital light processing (DLP) technique was used to fabricate oral dosage forms of different shapes with zolpidem tartrate (ZT), incorporated within its therapeutic range. Formulation factors, such as poly(ethylene glycol) diacrylate (PEGDA) and poly(ethylene glycol) 400 (PEG 400) ratio, as well as water content, were varied in combination with the surface area/volume (SA/V) ratio to achieve immediate drug release. Hypromellose (HPMC) was used as a stabilizing agent of photoreactive suspensions in an attempt to prevent drug sedimentation and subsequent variations in drug content uniformity. Oral dosage forms with doses in the range from 0.15 mg to 6.37 mg, showing very rapid and rapid drug dissolution, were successfully fabricated, confirming the potential of this technique in drug manufacturing with the ability to provide flexible dose adjustments and desirable release profiles by varying formulation factors and geometry of 3D models. DSC (differential scanning calorimetry), XRPD (X-ray powder diffraction) and scanning electron microscopy (SEM) showed that ZT remained in a crystalline form within printed dosage forms and no interactions were found between ZT and polymers.
PB  - Elsevier
T2  - International journal of pharmaceutics
T1  - Formulation and characterization of immediate-release oral dosage forms with zolpidem tartrate fabricated by digital light processing (DLP) 3D printing technique
VL  - 624
DO  - 10.1016/j.ijpharm.2022.122046
ER  - 

@article{
author = "Adamov, Ivana and Stanojević, Gordana and Medarević, Đorđe and Ivković, Branka and Kočović, David and Mirković, Dušica and Ibrić, Svetlana",
year = "2022",
abstract = "The introduction of three-dimensional (3D) printing in the pharmaceutical field has made great strides towards innovations in the way drugs are designed and manufactured. In this study, digital light processing (DLP) technique was used to fabricate oral dosage forms of different shapes with zolpidem tartrate (ZT), incorporated within its therapeutic range. Formulation factors, such as poly(ethylene glycol) diacrylate (PEGDA) and poly(ethylene glycol) 400 (PEG 400) ratio, as well as water content, were varied in combination with the surface area/volume (SA/V) ratio to achieve immediate drug release. Hypromellose (HPMC) was used as a stabilizing agent of photoreactive suspensions in an attempt to prevent drug sedimentation and subsequent variations in drug content uniformity. Oral dosage forms with doses in the range from 0.15 mg to 6.37 mg, showing very rapid and rapid drug dissolution, were successfully fabricated, confirming the potential of this technique in drug manufacturing with the ability to provide flexible dose adjustments and desirable release profiles by varying formulation factors and geometry of 3D models. DSC (differential scanning calorimetry), XRPD (X-ray powder diffraction) and scanning electron microscopy (SEM) showed that ZT remained in a crystalline form within printed dosage forms and no interactions were found between ZT and polymers.",
publisher = "Elsevier",
journal = "International journal of pharmaceutics",
title = "Formulation and characterization of immediate-release oral dosage forms with zolpidem tartrate fabricated by digital light processing (DLP) 3D printing technique",
volume = "624",
doi = "10.1016/j.ijpharm.2022.122046"
}

Adamov, I., Stanojević, G., Medarević, Đ., Ivković, B., Kočović, D., Mirković, D.,& Ibrić, S.. (2022). Formulation and characterization of immediate-release oral dosage forms with zolpidem tartrate fabricated by digital light processing (DLP) 3D printing technique. in International journal of pharmaceutics
Elsevier., 624.
https://doi.org/10.1016/j.ijpharm.2022.122046

Adamov I, Stanojević G, Medarević Đ, Ivković B, Kočović D, Mirković D, Ibrić S. Formulation and characterization of immediate-release oral dosage forms with zolpidem tartrate fabricated by digital light processing (DLP) 3D printing technique. in International journal of pharmaceutics. 2022;624.
doi:10.1016/j.ijpharm.2022.122046 .

Adamov, Ivana, Stanojević, Gordana, Medarević, Đorđe, Ivković, Branka, Kočović, David, Mirković, Dušica, Ibrić, Svetlana, "Formulation and characterization of immediate-release oral dosage forms with zolpidem tartrate fabricated by digital light processing (DLP) 3D printing technique" in International journal of pharmaceutics, 624 (2022),
https://doi.org/10.1016/j.ijpharm.2022.122046 . .

TY  - JOUR
AU  - Osmanović Omerdić, Ehlimana
AU  - Alagić-Džambić, Larisa
AU  - Krstić, Marko
AU  - Pašić-Kulenović, Maja
AU  - Medarević, Đorđe
AU  - Ivković, Branka
AU  - Vasiljević, Dragana
PY  - 2022
UR  - https://farfar.pharmacy.bg.ac.rs/handle/123456789/4085
AB  - Formulation of solid dispersions (SDs), in which the drug substance is dissolved or dispersed inside a polymer matrix, is one of the modern approaches to increase the solubility and dissolution rate of poorly soluble active pharmaceutical ingredients (APIs), such as clopidogrel. In the form of a free base, clopidogrel is unstable under increased both high moisture and temperature, so it is most often used as its salt form, clopidogrel hydrogen sulfate (CHS).The aim of this study was the formulation, characterization, and long-term stability investigation of CHS solid dispersions, prepared with four different hydrophilic polymers (poloxamer 407, macrogol 6000, povidone, copovidone) in five API/polymer ratios (1:1, 1:2, 1:3, 1:5, 1:9). SDs were prepared by the solvent evaporation method, employing ethanol (96% v/v) as a solvent. Initial results of the in vitro dissolution test showed an increase in the amount of dissolved CHS from all prepared SD samples compared to pure CHS, corresponding physical mixtures (PMs), and commercial tablets. SDs, prepared with poloxamer 407, macrogol 6000, and copovidone, at CHS/polymer ratios 1:5 and 1:9, notably increased the amount of dissolved CHS (> 80%, after 60 min), thus they were selected for further characterization. To assess the SDs long-term stability, in vitro dissolution studies, clopidogrel content determination, differential scanning calorimetry (DSC), and Fourier transform infrared spectroscopy (FT-IR) were performed initially and after 12 months of long-term stability studies under controlled conditions (25°C, 60% RH) meeting the ICH guideline Q1A (R2) requirements. The clopidogrel content in the selected samples was very similar at the beginning (96.13% to 99.93%) and at the end (95.98% to 99.86%) of the conducted test. DSC curves and FT-IR spectra of all SD samples after 12 months of stability study, showed the absence of CHS crystallization, which is an indication of good stability. However, the in vitro dissolution test showed a considerable reduction in CHS released from SDs with macrogol 6000. The amount of dissolved CHS from SDs with macrogol 6000 was initially 94.02% and 92.01%, and after 12 months of stability study, only 65.13% and 49.62%. In contrast, the amount of dissolved CHS from SDs prepared with poloxamer 407 and copovidone was very similar after 12 months of the stability study compared to the initial values. Results obtained indicated the great importance of the in vitro dissolution test in determining the long-term stability and quality of SDs.
PB  - NLM (Medline)
T2  - PloS one
T1  - Long-term stability of clopidogrel solid dispersions-Importance of in vitro dissolution test
VL  - 17
IS  - 4
DO  - 10.1371/journal.pone.0266237
ER  - 

@article{
author = "Osmanović Omerdić, Ehlimana and Alagić-Džambić, Larisa and Krstić, Marko and Pašić-Kulenović, Maja and Medarević, Đorđe and Ivković, Branka and Vasiljević, Dragana",
year = "2022",
abstract = "Formulation of solid dispersions (SDs), in which the drug substance is dissolved or dispersed inside a polymer matrix, is one of the modern approaches to increase the solubility and dissolution rate of poorly soluble active pharmaceutical ingredients (APIs), such as clopidogrel. In the form of a free base, clopidogrel is unstable under increased both high moisture and temperature, so it is most often used as its salt form, clopidogrel hydrogen sulfate (CHS).The aim of this study was the formulation, characterization, and long-term stability investigation of CHS solid dispersions, prepared with four different hydrophilic polymers (poloxamer 407, macrogol 6000, povidone, copovidone) in five API/polymer ratios (1:1, 1:2, 1:3, 1:5, 1:9). SDs were prepared by the solvent evaporation method, employing ethanol (96% v/v) as a solvent. Initial results of the in vitro dissolution test showed an increase in the amount of dissolved CHS from all prepared SD samples compared to pure CHS, corresponding physical mixtures (PMs), and commercial tablets. SDs, prepared with poloxamer 407, macrogol 6000, and copovidone, at CHS/polymer ratios 1:5 and 1:9, notably increased the amount of dissolved CHS (> 80%, after 60 min), thus they were selected for further characterization. To assess the SDs long-term stability, in vitro dissolution studies, clopidogrel content determination, differential scanning calorimetry (DSC), and Fourier transform infrared spectroscopy (FT-IR) were performed initially and after 12 months of long-term stability studies under controlled conditions (25°C, 60% RH) meeting the ICH guideline Q1A (R2) requirements. The clopidogrel content in the selected samples was very similar at the beginning (96.13% to 99.93%) and at the end (95.98% to 99.86%) of the conducted test. DSC curves and FT-IR spectra of all SD samples after 12 months of stability study, showed the absence of CHS crystallization, which is an indication of good stability. However, the in vitro dissolution test showed a considerable reduction in CHS released from SDs with macrogol 6000. The amount of dissolved CHS from SDs with macrogol 6000 was initially 94.02% and 92.01%, and after 12 months of stability study, only 65.13% and 49.62%. In contrast, the amount of dissolved CHS from SDs prepared with poloxamer 407 and copovidone was very similar after 12 months of the stability study compared to the initial values. Results obtained indicated the great importance of the in vitro dissolution test in determining the long-term stability and quality of SDs.",
publisher = "NLM (Medline)",
journal = "PloS one",
title = "Long-term stability of clopidogrel solid dispersions-Importance of in vitro dissolution test",
volume = "17",
number = "4",
doi = "10.1371/journal.pone.0266237"
}

Osmanović Omerdić, E., Alagić-Džambić, L., Krstić, M., Pašić-Kulenović, M., Medarević, Đ., Ivković, B.,& Vasiljević, D.. (2022). Long-term stability of clopidogrel solid dispersions-Importance of in vitro dissolution test. in PloS one
NLM (Medline)., 17(4).
https://doi.org/10.1371/journal.pone.0266237

Osmanović Omerdić E, Alagić-Džambić L, Krstić M, Pašić-Kulenović M, Medarević Đ, Ivković B, Vasiljević D. Long-term stability of clopidogrel solid dispersions-Importance of in vitro dissolution test. in PloS one. 2022;17(4).
doi:10.1371/journal.pone.0266237 .

Osmanović Omerdić, Ehlimana, Alagić-Džambić, Larisa, Krstić, Marko, Pašić-Kulenović, Maja, Medarević, Đorđe, Ivković, Branka, Vasiljević, Dragana, "Long-term stability of clopidogrel solid dispersions-Importance of in vitro dissolution test" in PloS one, 17, no. 4 (2022),
https://doi.org/10.1371/journal.pone.0266237 . .

TY  - JOUR
AU  - Nikolić, Nenad
AU  - Miletić, Tijana
AU  - Kovačević, Jovana
AU  - Medarević, Đorđe
AU  - Ibrić, Svetlana
PY  - 2022
UR  - https://farfar.pharmacy.bg.ac.rs/handle/123456789/4407
AB  - Compaction simulators are designed as machines which can provide an in-depth analysis
of the powder compaction process. Characterization of the powder compression and compaction
process, as well as material characterization, play an important role in the formulation and
manufacturing process design and development, as well as in creating a strong knowledge basis
for the scale-up of the tablet compression and troubleshooting in further stages of the product
lifecycle. Although compaction simulators are designed to simulate the compression process on
high-speed tablet-presses, with the advantages of a small quantity of material needed and highly
sophisticated instrumentation, there are certain limitations in the extrapolation of the process
parameters from these machines to high-speed rotary tablet presses. However, the advantage of
the use of compaction simulators for studying basic compression and compaction mechanisms,
identification of critical material attributes and critical process parameters ranges, and their
relations with tablet characteristics and critical quality attributes of pharmaceutical products is
clear, compared to the use of small excentre tablet presses, and complementary to the use of small
rotary tablet presses.
This scientific paper provides an overview and examples of the different advantages
provided by the instrumentation of compaction simulators, including certain limitations in their
exploitation.
AB  - Simulatori kompaktiranja su uređaji dizajnirani da omoguće dublju analizu procesa komprimovanja praškova. Karakterizacija procesa kompresije i kompakcije praškova, kao i karakterizacija materijala, ima važnu ulogu u dizajnu i razvoju formulacije i proizvodnog procesa tableta, kao i za kreiranje snažne baze za transfer proizvodnog procesa komprimovanja tableta na proizvodnu opremu i rešavanje problema u proizvodnim procesima u kasnijim fazama životnog ciklusa proizvoda. Iako su simulatori kompaktiranja dizajnirani da simuliraju proces kompresije na tablet-presama visoke brzine, obezbeđujući prednost korišćenja manjih količina materijala i visoko sofisticirane instrumentacije, postoje određena ograničenja u ekstrapolaciji procesnih parametara sa ovih mašina na tablet-prese visokih brzina. Međutim, prednosti upotrebe simulatora kompaktiranja za proučavanje osnovnih mehanizama kompresije i kompaktiranja, identifikaciju kritičnih karakteristika materijala i opsega kritičnih procesnih parametara, kao i njihovih relacija sa karakteristikama tableta, i kritičnim karakteristikama farmaceutskih proizvoda su očigledne, u poređenju sa korišćenjem malih ekscenter tablet presa, i komplementarne sa upotrebom manjih rotacionih tablet presa. U ovom radu je prikazan pregled i primeri različitih prednosti omogućenih nivoom instrumentacije simulatora kompaktiranja, uključujući i ograničenja u njihovoj eksploataciji.
PB  - Pharmaceutical Association of Serbia
T2  - Arhiv za farmaciju
T1  - Usage of compaction simulators for the powder compression characterization – advantages and limitations
T1  - Upotreba simulatora kompaktiranja za karakterizaciju kompresije praškova - prednosti i ograničenja
VL  - 72
IS  - 6
SP  - 546
EP  - 565
DO  - 10.5937/arhfarm72-41301
ER  - 

@article{
author = "Nikolić, Nenad and Miletić, Tijana and Kovačević, Jovana and Medarević, Đorđe and Ibrić, Svetlana",
year = "2022",
abstract = "Compaction simulators are designed as machines which can provide an in-depth analysis
of the powder compaction process. Characterization of the powder compression and compaction
process, as well as material characterization, play an important role in the formulation and
manufacturing process design and development, as well as in creating a strong knowledge basis
for the scale-up of the tablet compression and troubleshooting in further stages of the product
lifecycle. Although compaction simulators are designed to simulate the compression process on
high-speed tablet-presses, with the advantages of a small quantity of material needed and highly
sophisticated instrumentation, there are certain limitations in the extrapolation of the process
parameters from these machines to high-speed rotary tablet presses. However, the advantage of
the use of compaction simulators for studying basic compression and compaction mechanisms,
identification of critical material attributes and critical process parameters ranges, and their
relations with tablet characteristics and critical quality attributes of pharmaceutical products is
clear, compared to the use of small excentre tablet presses, and complementary to the use of small
rotary tablet presses.
This scientific paper provides an overview and examples of the different advantages
provided by the instrumentation of compaction simulators, including certain limitations in their
exploitation., Simulatori kompaktiranja su uređaji dizajnirani da omoguće dublju analizu procesa komprimovanja praškova. Karakterizacija procesa kompresije i kompakcije praškova, kao i karakterizacija materijala, ima važnu ulogu u dizajnu i razvoju formulacije i proizvodnog procesa tableta, kao i za kreiranje snažne baze za transfer proizvodnog procesa komprimovanja tableta na proizvodnu opremu i rešavanje problema u proizvodnim procesima u kasnijim fazama životnog ciklusa proizvoda. Iako su simulatori kompaktiranja dizajnirani da simuliraju proces kompresije na tablet-presama visoke brzine, obezbeđujući prednost korišćenja manjih količina materijala i visoko sofisticirane instrumentacije, postoje određena ograničenja u ekstrapolaciji procesnih parametara sa ovih mašina na tablet-prese visokih brzina. Međutim, prednosti upotrebe simulatora kompaktiranja za proučavanje osnovnih mehanizama kompresije i kompaktiranja, identifikaciju kritičnih karakteristika materijala i opsega kritičnih procesnih parametara, kao i njihovih relacija sa karakteristikama tableta, i kritičnim karakteristikama farmaceutskih proizvoda su očigledne, u poređenju sa korišćenjem malih ekscenter tablet presa, i komplementarne sa upotrebom manjih rotacionih tablet presa. U ovom radu je prikazan pregled i primeri različitih prednosti omogućenih nivoom instrumentacije simulatora kompaktiranja, uključujući i ograničenja u njihovoj eksploataciji.",
publisher = "Pharmaceutical Association of Serbia",
journal = "Arhiv za farmaciju",
title = "Usage of compaction simulators for the powder compression characterization – advantages and limitations, Upotreba simulatora kompaktiranja za karakterizaciju kompresije praškova - prednosti i ograničenja",
volume = "72",
number = "6",
pages = "546-565",
doi = "10.5937/arhfarm72-41301"
}

Nikolić, N., Miletić, T., Kovačević, J., Medarević, Đ.,& Ibrić, S.. (2022). Usage of compaction simulators for the powder compression characterization – advantages and limitations. in Arhiv za farmaciju
Pharmaceutical Association of Serbia., 72(6), 546-565.
https://doi.org/10.5937/arhfarm72-41301

Nikolić N, Miletić T, Kovačević J, Medarević Đ, Ibrić S. Usage of compaction simulators for the powder compression characterization – advantages and limitations. in Arhiv za farmaciju. 2022;72(6):546-565.
doi:10.5937/arhfarm72-41301 .

Nikolić, Nenad, Miletić, Tijana, Kovačević, Jovana, Medarević, Đorđe, Ibrić, Svetlana, "Usage of compaction simulators for the powder compression characterization – advantages and limitations" in Arhiv za farmaciju, 72, no. 6 (2022):546-565,
https://doi.org/10.5937/arhfarm72-41301 . .

TY  - JOUR
AU  - Madžarević, Marijana
AU  - Medarević, Đorđe
AU  - Pavlović, Stefan
AU  - Ivković, Branka
AU  - Đuriš, Jelena
AU  - Ibrić, Svetlana
PY  - 2021
UR  - https://farfar.pharmacy.bg.ac.rs/handle/123456789/5544
AB  - Selective laser sintering (SLS) is a rapid prototyping technique for the production of
three-dimensional objects through selectively sintering powder-based layer materials. The aim
of the study was to investigate the effect of energy density (ED) and formulation factors on the
printability and characteristics of SLS irbesartan tablets. The correlation between formulation factors,
ED, and printability was obtained using a decision tree model with an accuracy of 80%. FT-IR
results revealed that there was no interaction between irbesartan and the applied excipients. DSC
results indicated that irbesartan was present in an amorphous form in printed tablets. ED had a
significant influence on tablets’ physical, mechanical, and morphological characteristics. Adding
lactose monohydrate enabled faster drug release while reducing the possibility for printing with
different laser speeds. However, formulations with crospovidone were printable with a wider range
of laser speeds. The adjustment of formulation and process parameters enabled the production of SLS
tablets with hydroxypropyl methylcellulose with complete release in less than 30 min. The results
suggest that a decision tree could be a useful tool for predicting the printability of pharmaceutical
formulations. Tailoring the characteristics of SLS irbesartan tablets by ED is possible; however,
it needs to be governed by the composition of the whole formulation.
PB  - MDPI
T2  - Pharmaceutics
T1  - Understanding the Effect of Energy Density and Formulation Factors on the Printability and Characteristics of SLS Irbesartan Tablets—Application of the Decision Tree Model
VL  - 13
IS  - 11
SP  - 1969
DO  - 10.3390/pharmaceutics13111969
ER  - 

@article{
author = "Madžarević, Marijana and Medarević, Đorđe and Pavlović, Stefan and Ivković, Branka and Đuriš, Jelena and Ibrić, Svetlana",
year = "2021",
abstract = "Selective laser sintering (SLS) is a rapid prototyping technique for the production of
three-dimensional objects through selectively sintering powder-based layer materials. The aim
of the study was to investigate the effect of energy density (ED) and formulation factors on the
printability and characteristics of SLS irbesartan tablets. The correlation between formulation factors,
ED, and printability was obtained using a decision tree model with an accuracy of 80%. FT-IR
results revealed that there was no interaction between irbesartan and the applied excipients. DSC
results indicated that irbesartan was present in an amorphous form in printed tablets. ED had a
significant influence on tablets’ physical, mechanical, and morphological characteristics. Adding
lactose monohydrate enabled faster drug release while reducing the possibility for printing with
different laser speeds. However, formulations with crospovidone were printable with a wider range
of laser speeds. The adjustment of formulation and process parameters enabled the production of SLS
tablets with hydroxypropyl methylcellulose with complete release in less than 30 min. The results
suggest that a decision tree could be a useful tool for predicting the printability of pharmaceutical
formulations. Tailoring the characteristics of SLS irbesartan tablets by ED is possible; however,
it needs to be governed by the composition of the whole formulation.",
publisher = "MDPI",
journal = "Pharmaceutics",
title = "Understanding the Effect of Energy Density and Formulation Factors on the Printability and Characteristics of SLS Irbesartan Tablets—Application of the Decision Tree Model",
volume = "13",
number = "11",
pages = "1969",
doi = "10.3390/pharmaceutics13111969"
}

Madžarević, M., Medarević, Đ., Pavlović, S., Ivković, B., Đuriš, J.,& Ibrić, S.. (2021). Understanding the Effect of Energy Density and Formulation Factors on the Printability and Characteristics of SLS Irbesartan Tablets—Application of the Decision Tree Model. in Pharmaceutics
MDPI., 13(11), 1969.
https://doi.org/10.3390/pharmaceutics13111969

Madžarević M, Medarević Đ, Pavlović S, Ivković B, Đuriš J, Ibrić S. Understanding the Effect of Energy Density and Formulation Factors on the Printability and Characteristics of SLS Irbesartan Tablets—Application of the Decision Tree Model. in Pharmaceutics. 2021;13(11):1969.
doi:10.3390/pharmaceutics13111969 .

Madžarević, Marijana, Medarević, Đorđe, Pavlović, Stefan, Ivković, Branka, Đuriš, Jelena, Ibrić, Svetlana, "Understanding the Effect of Energy Density and Formulation Factors on the Printability and Characteristics of SLS Irbesartan Tablets—Application of the Decision Tree Model" in Pharmaceutics, 13, no. 11 (2021):1969,
https://doi.org/10.3390/pharmaceutics13111969 . .

TY  - JOUR
AU  - Ćirić, Ana
AU  - Medarević, Đorđe
AU  - Čalija, Bojan
AU  - Dobričić, Vladimir
AU  - Rmandić, Milena
AU  - Barudžija, Tanja
AU  - Malenović, Anđelija
AU  - Đekić, Ljiljana
PY  - 2021
UR  - https://farfar.pharmacy.bg.ac.rs/handle/123456789/3759
AB  - The effect of the entrapment procedure of a poorly water soluble drug (ibuprofen) on physicochemical and drug release performances of chitosan/xanthan polyelectrolyte complexes (PECs) was investigated to achieve controlled drug release as the ultimate goal. The formation of PECs for two drug entrapment procedures (before or after the mixing of polymers) at pH 4.6 and 5.6 and three chitosan-to-xanthan mass ratios (1:1, 1:2 and 1:3) was observed by continuous decrease in conductivity during the PECs formation and increased apparent viscosity and hysteresis values. The most extensive crosslinking was observed with ibuprofen added before the PECs formation at pH 4.6 and chitosan-to-xanthan mass ratio 1:1. The PECs prepared at polymers' mass ratios 1:2 and 1:3 had higher yield and drug entrapment efficiency. DSC and FT-IR analysis confirmed ibuprofen entrapment in PECs and the partial disruption of its crystallinity. All ibuprofen release profiles were similar, with 60–70% of drug released after 12 h, mainly by diffusion, but erosion and polymer chain relaxation were also included. Potentially optimal can be considered the PEC prepared at pH 4.6, ibuprofen entrapped before the mixing of polymers at chitosan-to-xanthan mass ratio 1:2, which provided controlled drug release by zero-order kinetics, high yield, and drug entrapment efficiency.
PB  - Elsevier B.V.
T2  - International Journal of Biological Macromolecules
T1  - Effect of ibuprofen entrapment procedure on physicochemical and controlled drug release performances of chitosan/xanthan gum polyelectrolyte complexes
VL  - 167
SP  - 547
EP  - 558
DO  - 10.1016/j.ijbiomac.2020.11.201
ER  - 

@article{
author = "Ćirić, Ana and Medarević, Đorđe and Čalija, Bojan and Dobričić, Vladimir and Rmandić, Milena and Barudžija, Tanja and Malenović, Anđelija and Đekić, Ljiljana",
year = "2021",
abstract = "The effect of the entrapment procedure of a poorly water soluble drug (ibuprofen) on physicochemical and drug release performances of chitosan/xanthan polyelectrolyte complexes (PECs) was investigated to achieve controlled drug release as the ultimate goal. The formation of PECs for two drug entrapment procedures (before or after the mixing of polymers) at pH 4.6 and 5.6 and three chitosan-to-xanthan mass ratios (1:1, 1:2 and 1:3) was observed by continuous decrease in conductivity during the PECs formation and increased apparent viscosity and hysteresis values. The most extensive crosslinking was observed with ibuprofen added before the PECs formation at pH 4.6 and chitosan-to-xanthan mass ratio 1:1. The PECs prepared at polymers' mass ratios 1:2 and 1:3 had higher yield and drug entrapment efficiency. DSC and FT-IR analysis confirmed ibuprofen entrapment in PECs and the partial disruption of its crystallinity. All ibuprofen release profiles were similar, with 60–70% of drug released after 12 h, mainly by diffusion, but erosion and polymer chain relaxation were also included. Potentially optimal can be considered the PEC prepared at pH 4.6, ibuprofen entrapped before the mixing of polymers at chitosan-to-xanthan mass ratio 1:2, which provided controlled drug release by zero-order kinetics, high yield, and drug entrapment efficiency.",
publisher = "Elsevier B.V.",
journal = "International Journal of Biological Macromolecules",
title = "Effect of ibuprofen entrapment procedure on physicochemical and controlled drug release performances of chitosan/xanthan gum polyelectrolyte complexes",
volume = "167",
pages = "547-558",
doi = "10.1016/j.ijbiomac.2020.11.201"
}

Ćirić, A., Medarević, Đ., Čalija, B., Dobričić, V., Rmandić, M., Barudžija, T., Malenović, A.,& Đekić, L.. (2021). Effect of ibuprofen entrapment procedure on physicochemical and controlled drug release performances of chitosan/xanthan gum polyelectrolyte complexes. in International Journal of Biological Macromolecules
Elsevier B.V.., 167, 547-558.
https://doi.org/10.1016/j.ijbiomac.2020.11.201

Ćirić A, Medarević Đ, Čalija B, Dobričić V, Rmandić M, Barudžija T, Malenović A, Đekić L. Effect of ibuprofen entrapment procedure on physicochemical and controlled drug release performances of chitosan/xanthan gum polyelectrolyte complexes. in International Journal of Biological Macromolecules. 2021;167:547-558.
doi:10.1016/j.ijbiomac.2020.11.201 .

Ćirić, Ana, Medarević, Đorđe, Čalija, Bojan, Dobričić, Vladimir, Rmandić, Milena, Barudžija, Tanja, Malenović, Anđelija, Đekić, Ljiljana, "Effect of ibuprofen entrapment procedure on physicochemical and controlled drug release performances of chitosan/xanthan gum polyelectrolyte complexes" in International Journal of Biological Macromolecules, 167 (2021):547-558,
https://doi.org/10.1016/j.ijbiomac.2020.11.201 . .

TY  - CONF
AU  - Pešić, Nikola
AU  - Dapčević, Aleksandra
AU  - Ivković, Branka
AU  - Barudžija, Tanja
AU  - Krkobabić, Mirjana
AU  - Ibrić, Svetlana
AU  - Medarević, Đorđe
PY  - 2021
UR  - https://farfar.pharmacy.bg.ac.rs/handle/123456789/5327
AB  - INTRODUCTION
The development of formulations with amorphous form of drug is one of the most commonly used approaches for improving solubility and bioavailability of poorly soluble drugs. Solid dispersions with different hydrophilic polymers have been widely investigated during the last decades as an approach for development of stable formulations with amorphous drug. However, high weight percentage of polymer is usually required to ensure molecular mixing with drug and stability against drug recrystallization, making difficult formulation of final dosage form [1]. In the last years, formulations of co-amorphous systems, where amorphous drug is stabilized with low molecular weight components (drug or excipient) have been successfully used for improving solubility and bioavailability of poorly soluble drugs, with overcoming limitations of solid dispersions [2]. This study investigated effect of three amino acids (AAs) on amorphization of carvedilol (CRV) by dry milling process, with the overall aim to improve CRV dissolution.
EXPERIMENTAL METHODS
Materials
CRV (Hemofarm a.d., Serbia) was used as a model poorly soluble drug. L-tryptophan (TRY, Carl Roth, Germany), L-phenylalanine (PHE, Carl Roth, Germany) and L-lysine (LYS, Acros Organics, Belgium) were used as AAs.
Samples preparation and physicochemical characterization
Mixture of CRV and each of AAs in CRV:AAs molar ratios 1:0.5, 1:1 and 1:2 were placed in 125 ml stainless steel milling jar and subject to milling in high-energy planetary ball mill (PM 100, Retch, Germany) during 4 h, with 30 min break after 2 h. Milling was performed using 10 milling balls of 10 mm diameter with rotation speed of mill of 400 rpm.
Changes of CRV and AAs physical state due to milling were assessed by Powder X-ray Diffraction (PXRD, Philips PW1050, The Netherlands) and Differential Scanning Calorimetry (DSC, DSC 1, Mettler Toledo, Germany). In vitro dissolution testing was performed under non-sink conditions using rotating paddle apparatus (Erweka DT70, Erweka, Germany). Samples containing 100 mg of CRV were tested in 250 ml of phosphate buffer (pH=6.8) during
8 h, with paddle rotation speed of 50 rpm. Concentration of dissolved CRV was determined by HPLC (Dionex Ultimate 3000, Thermo scientific, USA). Area under dissolution curve (AUC) was calculated for each formulation and compared with AUC of CRV dissolution profile.
RESULTS AND DISCUSSION
Presence of diffraction peaks at 6.0, 15.0, 17.65, 18.55 and 24.5° 2θ and sharp melting endotherm at 116.6 °C confirmed that raw CRV was present in crystalline polymorph form II [3]. Significant reduction in crystallinity was observed for all samples prepared with TRY and PHE, while there were no peaks of CRV and AA on the PXRD pattern of CRV:TRY 1:2 sample. This was confirmed by the DSC analysis, where melting peaks of CRV and AAs were present on the thermograms of all samples except CRV:TRY 1:2 sample. This sample showed only exotherm at 102 °C due to recrystallization of TRY, followed by its melting at 266 °C, confirming CRV amorphization induced by milling. High crystallinity on PXRD patterns of all samples milled with LYS, together with the presence of melting peaks of both CRV and AA on the DSC thermograms, showed that LYS was the least suitable AA for amorphization of CRV. Despite that TRY and PHE induced partial or complete amorphization of CRV, these AAs were less efficient in improving dissolution of CRV compared to LYS. The highest supersaturation of CRV was achieved from CRV:LYS 1:1 sample with almost 3 times higher AUC compared to pure CRV. It is evident that maximum CRV concentration from this sample was reached in the first 90 min and is maintained during the entire test. Although similar CRV concentration was achieved after 60 min for CRV:LYS 1:2 sample, it is evident that CRV concentration started to decrease after this time point.
CONCLUSION
Complete amorphization was achieved by milling of only CRV:TRY 1:2 mixture, while significant decrease in crystallinity was observed for other samples milled with TRY and PHE. Although milling of CRV with LYS resulted in samples with the highest crystallinity, samples prepared with this AA in 1:1 and 1:2 molar ratios were the most efficient in providing CRV supersaturation. CRV:LYS 1:1 molar ratio can be considered as optimal, as achieved supersaturation was maintained during 8 h.
PB  - International Association for Pharmaceutical Technology, Mainz, Germany
C3  - 12th World Meeting on Pharmaceutics, Biopharmaceutics and Pharmaceutical Technology, 11-14 May 2021, Vienna, Austria, Virtual meeting
T1  - Evaluation of potential of amino acids for amorphization and dissolution improvement of carvedilol
SP  - 1
EP  - 2
UR  - https://hdl.handle.net/21.15107/rcub_farfar_5327
ER  - 

@conference{
author = "Pešić, Nikola and Dapčević, Aleksandra and Ivković, Branka and Barudžija, Tanja and Krkobabić, Mirjana and Ibrić, Svetlana and Medarević, Đorđe",
year = "2021",
abstract = "INTRODUCTION
The development of formulations with amorphous form of drug is one of the most commonly used approaches for improving solubility and bioavailability of poorly soluble drugs. Solid dispersions with different hydrophilic polymers have been widely investigated during the last decades as an approach for development of stable formulations with amorphous drug. However, high weight percentage of polymer is usually required to ensure molecular mixing with drug and stability against drug recrystallization, making difficult formulation of final dosage form [1]. In the last years, formulations of co-amorphous systems, where amorphous drug is stabilized with low molecular weight components (drug or excipient) have been successfully used for improving solubility and bioavailability of poorly soluble drugs, with overcoming limitations of solid dispersions [2]. This study investigated effect of three amino acids (AAs) on amorphization of carvedilol (CRV) by dry milling process, with the overall aim to improve CRV dissolution.
EXPERIMENTAL METHODS
Materials
CRV (Hemofarm a.d., Serbia) was used as a model poorly soluble drug. L-tryptophan (TRY, Carl Roth, Germany), L-phenylalanine (PHE, Carl Roth, Germany) and L-lysine (LYS, Acros Organics, Belgium) were used as AAs.
Samples preparation and physicochemical characterization
Mixture of CRV and each of AAs in CRV:AAs molar ratios 1:0.5, 1:1 and 1:2 were placed in 125 ml stainless steel milling jar and subject to milling in high-energy planetary ball mill (PM 100, Retch, Germany) during 4 h, with 30 min break after 2 h. Milling was performed using 10 milling balls of 10 mm diameter with rotation speed of mill of 400 rpm.
Changes of CRV and AAs physical state due to milling were assessed by Powder X-ray Diffraction (PXRD, Philips PW1050, The Netherlands) and Differential Scanning Calorimetry (DSC, DSC 1, Mettler Toledo, Germany). In vitro dissolution testing was performed under non-sink conditions using rotating paddle apparatus (Erweka DT70, Erweka, Germany). Samples containing 100 mg of CRV were tested in 250 ml of phosphate buffer (pH=6.8) during
8 h, with paddle rotation speed of 50 rpm. Concentration of dissolved CRV was determined by HPLC (Dionex Ultimate 3000, Thermo scientific, USA). Area under dissolution curve (AUC) was calculated for each formulation and compared with AUC of CRV dissolution profile.
RESULTS AND DISCUSSION
Presence of diffraction peaks at 6.0, 15.0, 17.65, 18.55 and 24.5° 2θ and sharp melting endotherm at 116.6 °C confirmed that raw CRV was present in crystalline polymorph form II [3]. Significant reduction in crystallinity was observed for all samples prepared with TRY and PHE, while there were no peaks of CRV and AA on the PXRD pattern of CRV:TRY 1:2 sample. This was confirmed by the DSC analysis, where melting peaks of CRV and AAs were present on the thermograms of all samples except CRV:TRY 1:2 sample. This sample showed only exotherm at 102 °C due to recrystallization of TRY, followed by its melting at 266 °C, confirming CRV amorphization induced by milling. High crystallinity on PXRD patterns of all samples milled with LYS, together with the presence of melting peaks of both CRV and AA on the DSC thermograms, showed that LYS was the least suitable AA for amorphization of CRV. Despite that TRY and PHE induced partial or complete amorphization of CRV, these AAs were less efficient in improving dissolution of CRV compared to LYS. The highest supersaturation of CRV was achieved from CRV:LYS 1:1 sample with almost 3 times higher AUC compared to pure CRV. It is evident that maximum CRV concentration from this sample was reached in the first 90 min and is maintained during the entire test. Although similar CRV concentration was achieved after 60 min for CRV:LYS 1:2 sample, it is evident that CRV concentration started to decrease after this time point.
CONCLUSION
Complete amorphization was achieved by milling of only CRV:TRY 1:2 mixture, while significant decrease in crystallinity was observed for other samples milled with TRY and PHE. Although milling of CRV with LYS resulted in samples with the highest crystallinity, samples prepared with this AA in 1:1 and 1:2 molar ratios were the most efficient in providing CRV supersaturation. CRV:LYS 1:1 molar ratio can be considered as optimal, as achieved supersaturation was maintained during 8 h.",
publisher = "International Association for Pharmaceutical Technology, Mainz, Germany",
journal = "12th World Meeting on Pharmaceutics, Biopharmaceutics and Pharmaceutical Technology, 11-14 May 2021, Vienna, Austria, Virtual meeting",
title = "Evaluation of potential of amino acids for amorphization and dissolution improvement of carvedilol",
pages = "1-2",
url = "https://hdl.handle.net/21.15107/rcub_farfar_5327"
}

Pešić, N., Dapčević, A., Ivković, B., Barudžija, T., Krkobabić, M., Ibrić, S.,& Medarević, Đ.. (2021). Evaluation of potential of amino acids for amorphization and dissolution improvement of carvedilol. in 12th World Meeting on Pharmaceutics, Biopharmaceutics and Pharmaceutical Technology, 11-14 May 2021, Vienna, Austria, Virtual meeting
International Association for Pharmaceutical Technology, Mainz, Germany., 1-2.
https://hdl.handle.net/21.15107/rcub_farfar_5327

Pešić N, Dapčević A, Ivković B, Barudžija T, Krkobabić M, Ibrić S, Medarević Đ. Evaluation of potential of amino acids for amorphization and dissolution improvement of carvedilol. in 12th World Meeting on Pharmaceutics, Biopharmaceutics and Pharmaceutical Technology, 11-14 May 2021, Vienna, Austria, Virtual meeting. 2021;:1-2.
https://hdl.handle.net/21.15107/rcub_farfar_5327 .

Pešić, Nikola, Dapčević, Aleksandra, Ivković, Branka, Barudžija, Tanja, Krkobabić, Mirjana, Ibrić, Svetlana, Medarević, Đorđe, "Evaluation of potential of amino acids for amorphization and dissolution improvement of carvedilol" in 12th World Meeting on Pharmaceutics, Biopharmaceutics and Pharmaceutical Technology, 11-14 May 2021, Vienna, Austria, Virtual meeting (2021):1-2,
https://hdl.handle.net/21.15107/rcub_farfar_5327 .

TY  - CONF
AU  - Medarević, Đorđe
AU  - Dobričić, Vladimir
AU  - Krkobabić, Mirjana
AU  - Pešić, Nikola
AU  - Ibrić, Svetlana
PY  - 2021
UR  - https://farfar.pharmacy.bg.ac.rs/handle/123456789/5326
AB  - INTRODUCTION
Formulation of solid dispersions (SDs) with water soluble polymers is one of the most efficient approaches for improving the dissolution rate of poorly soluble drugs. However, this formulation approach might not always be effective in improving the dissolution rate of drugs, especially those with pH-dependent solubility (1). The addition of alkalizers or acidifiers can solve this problem by changing pH in the near vicinity of drug particle surface, (microenvironmental pH) to the range where drug easily dissolves (2). This study evaluated the potential of several alkalizers for improving the dissolution rate of weakly acidic drug valsartan (VAL) from SDs prepared with hydrophilic polymers.
EXPERIMENTAL METHODS
Materials
VAL (Hemofarm a.d., Serbia) was used as a model poorly soluble drug. Hypromellose (HPMC E5, MethocelTM E5 LV premium, Dow Chemicals, USA) and polyvinylpyrrolidone (PVPK25, Kollidon® 25, BASF, Germany) were used as hydrophilic polymers for SDs preparation. Calcium oxide (CaO), magnesium oxide (MgO), sodium carbonate (Na2CO3) and meglumine (MEG) were used as alkalizers in solid dispersions.
SDs preparation
SDs were prepared in VAL:polymer:alkalizer (V:P:A) weight ratios 1:2:0.5, 1:2:1 and 1:2:2 (Table 1.). Additionally, binary SDs were prepared with VAL and polymer, but without alkalizer. VAL and polymer were dissolved in absolute ethanol on a magnetic stirred followed by dispersion of alkalizer. Ethanol was evaporated from dispersion using rotary evaporator (Büchi Rotavapor®, Büchi Labortechnik AG, Switzerland) at 50 °C. After further vacuum drying, mass was pulverized and sieved through sieve 355 μm.
SDs characterization
FT-IR spectroscopy (Nicolet iS10, Thermo Scientific, USA) was used to detect the presence of intermolecular interactions between drug, polymer and alkalizer. In vitro drug dissolution testing was performed using a rotating paddle apparatus in 900 ml of 0.1 M HCl as a dissolution medium, due to poor solubility of VAL in this medium. Microenvironmental pH (pHM) was estimated by measuring of pH of concentrated suspension of SD as an indicator of pH near the surface of drug particles.
RESULTS AND DISCUSSION
Slow and incomplete dissolution of VAL was observed from binary SDs with either PVP or HPMC. The addition of alkalizer resulted in a significantly improved VAL dissolution rate from SDs with both polymers, with faster VAL release from SDs with PVP. Na2CO3 showed the best performance in improving VAL dissolution rate amongst all tested alkalizers. Desired immediate release of VAL (>80% of VAL dissolved after 30 min) was achieved only from formulations SD8 and SD12 prepared with Na2CO3 in 1:2:1 and 1:2:2 V:P:A ratios, and also from formulation SD6 prepared with CaO in 1:2:1 V:P:A ratio). The addition of all alkalizers resulted in higher pHM (Table 1), independently of polymer used, but with considerable differences amongst tested alkalizers. The highest efficiency of Na2CO3 in improving VAL dissolution rate was not correlated with measured pHM, as higher pHM was measured for samples with CaO and MgO. However, the lowest pHM measured for samples with MEG was in accordance with the lowest capacity of this alkalizer to improve VAL dissolution rate. Due to the fastest VAL release achieved, SDs with PVP K25 and CaO or Na2CO3 were further characterized by FT-IR spectroscopy to detect the presence of intermolecular interactions in comparison with binary VAL:PVP SD (SDP) and corresponding physical mixtures (PMs). Shifting and decrease in intensity of VAL absorption band at 1729 cm-1 (carboxyl C=O stretching) and disappearance of peak at 1599 cm-1 (amide C=O stretching) was observed on the spectra of binary VAL:PVP SD compared to PM of equivalent composition, indicating that both C=O groups of VAL can be involved in intermolecular interaction with PVP. The same region of FT-IR spectra was changed in the case of SDs with alkalizer, where peak at 1729 cm-1 disappeared, while peak at 1599 cm-1 was reduced in intensity. Therefore, the same kind of interactions was observed for both binary and ternary SDs, which cannot explain observed faster VAL dissolution rate from ternary SDs with alkalizer.
CONCLUSION
The addition of alkalizer resulted in significantly improved VAL dissolution rate from SDs prepared with HPMC and PVP, wherein Na2CO3 showed the best performance amongst all tested alkalizers. Since slightly higher pHM was achieved with CaO and MgO, higher efficiency of Na2CO3 can be ascribed to its higher solubility which enables generation of pores in SDs, while release of carbon dioxide facilitates dispersion of particles in the dissolution medium and reduces their tendency towards aggregation.
PB  - International Association for Pharmaceutical Technology, Mainz, Germany
C3  - 12th World Meeting on Pharmaceutics, Biopharmaceutics and Pharmaceutical Technology, 11-14 May 2021, Vienna, Austria, Virtual meeting
T1  - Microenvironmental pH-modified solid dispersions for improving dissolution rate of valsartan
SP  - 1
EP  - 2
UR  - https://hdl.handle.net/21.15107/rcub_farfar_5326
ER  - 

@conference{
author = "Medarević, Đorđe and Dobričić, Vladimir and Krkobabić, Mirjana and Pešić, Nikola and Ibrić, Svetlana",
year = "2021",
abstract = "INTRODUCTION
Formulation of solid dispersions (SDs) with water soluble polymers is one of the most efficient approaches for improving the dissolution rate of poorly soluble drugs. However, this formulation approach might not always be effective in improving the dissolution rate of drugs, especially those with pH-dependent solubility (1). The addition of alkalizers or acidifiers can solve this problem by changing pH in the near vicinity of drug particle surface, (microenvironmental pH) to the range where drug easily dissolves (2). This study evaluated the potential of several alkalizers for improving the dissolution rate of weakly acidic drug valsartan (VAL) from SDs prepared with hydrophilic polymers.
EXPERIMENTAL METHODS
Materials
VAL (Hemofarm a.d., Serbia) was used as a model poorly soluble drug. Hypromellose (HPMC E5, MethocelTM E5 LV premium, Dow Chemicals, USA) and polyvinylpyrrolidone (PVPK25, Kollidon® 25, BASF, Germany) were used as hydrophilic polymers for SDs preparation. Calcium oxide (CaO), magnesium oxide (MgO), sodium carbonate (Na2CO3) and meglumine (MEG) were used as alkalizers in solid dispersions.
SDs preparation
SDs were prepared in VAL:polymer:alkalizer (V:P:A) weight ratios 1:2:0.5, 1:2:1 and 1:2:2 (Table 1.). Additionally, binary SDs were prepared with VAL and polymer, but without alkalizer. VAL and polymer were dissolved in absolute ethanol on a magnetic stirred followed by dispersion of alkalizer. Ethanol was evaporated from dispersion using rotary evaporator (Büchi Rotavapor®, Büchi Labortechnik AG, Switzerland) at 50 °C. After further vacuum drying, mass was pulverized and sieved through sieve 355 μm.
SDs characterization
FT-IR spectroscopy (Nicolet iS10, Thermo Scientific, USA) was used to detect the presence of intermolecular interactions between drug, polymer and alkalizer. In vitro drug dissolution testing was performed using a rotating paddle apparatus in 900 ml of 0.1 M HCl as a dissolution medium, due to poor solubility of VAL in this medium. Microenvironmental pH (pHM) was estimated by measuring of pH of concentrated suspension of SD as an indicator of pH near the surface of drug particles.
RESULTS AND DISCUSSION
Slow and incomplete dissolution of VAL was observed from binary SDs with either PVP or HPMC. The addition of alkalizer resulted in a significantly improved VAL dissolution rate from SDs with both polymers, with faster VAL release from SDs with PVP. Na2CO3 showed the best performance in improving VAL dissolution rate amongst all tested alkalizers. Desired immediate release of VAL (>80% of VAL dissolved after 30 min) was achieved only from formulations SD8 and SD12 prepared with Na2CO3 in 1:2:1 and 1:2:2 V:P:A ratios, and also from formulation SD6 prepared with CaO in 1:2:1 V:P:A ratio). The addition of all alkalizers resulted in higher pHM (Table 1), independently of polymer used, but with considerable differences amongst tested alkalizers. The highest efficiency of Na2CO3 in improving VAL dissolution rate was not correlated with measured pHM, as higher pHM was measured for samples with CaO and MgO. However, the lowest pHM measured for samples with MEG was in accordance with the lowest capacity of this alkalizer to improve VAL dissolution rate. Due to the fastest VAL release achieved, SDs with PVP K25 and CaO or Na2CO3 were further characterized by FT-IR spectroscopy to detect the presence of intermolecular interactions in comparison with binary VAL:PVP SD (SDP) and corresponding physical mixtures (PMs). Shifting and decrease in intensity of VAL absorption band at 1729 cm-1 (carboxyl C=O stretching) and disappearance of peak at 1599 cm-1 (amide C=O stretching) was observed on the spectra of binary VAL:PVP SD compared to PM of equivalent composition, indicating that both C=O groups of VAL can be involved in intermolecular interaction with PVP. The same region of FT-IR spectra was changed in the case of SDs with alkalizer, where peak at 1729 cm-1 disappeared, while peak at 1599 cm-1 was reduced in intensity. Therefore, the same kind of interactions was observed for both binary and ternary SDs, which cannot explain observed faster VAL dissolution rate from ternary SDs with alkalizer.
CONCLUSION
The addition of alkalizer resulted in significantly improved VAL dissolution rate from SDs prepared with HPMC and PVP, wherein Na2CO3 showed the best performance amongst all tested alkalizers. Since slightly higher pHM was achieved with CaO and MgO, higher efficiency of Na2CO3 can be ascribed to its higher solubility which enables generation of pores in SDs, while release of carbon dioxide facilitates dispersion of particles in the dissolution medium and reduces their tendency towards aggregation.",
publisher = "International Association for Pharmaceutical Technology, Mainz, Germany",
journal = "12th World Meeting on Pharmaceutics, Biopharmaceutics and Pharmaceutical Technology, 11-14 May 2021, Vienna, Austria, Virtual meeting",
title = "Microenvironmental pH-modified solid dispersions for improving dissolution rate of valsartan",
pages = "1-2",
url = "https://hdl.handle.net/21.15107/rcub_farfar_5326"
}

Medarević, Đ., Dobričić, V., Krkobabić, M., Pešić, N.,& Ibrić, S.. (2021). Microenvironmental pH-modified solid dispersions for improving dissolution rate of valsartan. in 12th World Meeting on Pharmaceutics, Biopharmaceutics and Pharmaceutical Technology, 11-14 May 2021, Vienna, Austria, Virtual meeting
International Association for Pharmaceutical Technology, Mainz, Germany., 1-2.
https://hdl.handle.net/21.15107/rcub_farfar_5326

Medarević Đ, Dobričić V, Krkobabić M, Pešić N, Ibrić S. Microenvironmental pH-modified solid dispersions for improving dissolution rate of valsartan. in 12th World Meeting on Pharmaceutics, Biopharmaceutics and Pharmaceutical Technology, 11-14 May 2021, Vienna, Austria, Virtual meeting. 2021;:1-2.
https://hdl.handle.net/21.15107/rcub_farfar_5326 .

Medarević, Đorđe, Dobričić, Vladimir, Krkobabić, Mirjana, Pešić, Nikola, Ibrić, Svetlana, "Microenvironmental pH-modified solid dispersions for improving dissolution rate of valsartan" in 12th World Meeting on Pharmaceutics, Biopharmaceutics and Pharmaceutical Technology, 11-14 May 2021, Vienna, Austria, Virtual meeting (2021):1-2,
https://hdl.handle.net/21.15107/rcub_farfar_5326 .

TY  - CONF
AU  - Krkobabić, Mirjana
AU  - Pešić, Nikola
AU  - Boljević, Gordana
AU  - Medarević, Đorđe
AU  - Ibrić, Svetlana
PY  - 2021
UR  - https://farfar.pharmacy.bg.ac.rs/handle/123456789/5325
AB  - INTRODUCTION
Application of the 3D printing in pharmacy make possible production of small batches of solid dosage forms for oral administration (printlets) with different dose and release characteristics that can be customized to specific patient needs [1]. Digital light processing (DLP), one type of 3D printing technology, is based on a UV-triggered localized photopolymerization process of liquid resins [2]. The aim of this study was 3D printing from photoreactive dispersions with different amounts of solid phase and characterization of obtained printlets.
MATERIALS
Different photoreactive dispersions were prepared from poly(ethylene glycol) diacrylate 700 (PEGDA 700, Sigma-Aldrich, Japan), poly(ethylene glycol) 400 (PEG 400, Fagron, Netherlands), atomoxetine (kindly provided by Hemofarm AD, Vrsac, Serbia), diphenyl(2,4,6-trimethylbenzoyl) phosphine oxide (DPPO, Sigma-Aldrich, Germany).
Preparation of photoreactive dispersions
Atomoxetine was used as an active ingredient, while PEGDA was used as a photopolymer and DPPO as a photoinitiator in photoreactive dispersions. PEG 400 was used as an excipient to overcome very slow and incomplete drug release from printlets fabricated by photopolymerization using DLP technology. The ratio of PEGDA and PEG 400 was constant in all formulations (3:1), and content of atomoxetine was varied from 5% to 27.5% (Table 1). 30 g of each formulation was prepared by mixing on the magnetic stirrer for 15 minutes, protected from the light.
3D printing of atomoxetine printlets
The templates used for printlets were designed by Autodesk Fusion 360 software and exported as a stereolithography file (.stl) into Creation Workshop X 1.2.1 software. All printlets were fabricated using DLP printer Duplicator 7 (Wanhao, Zhejiang, China). The selected shape was cylinder (8 mm diameter and 2 mm height). Printlets containing 5.00% of atomoxetine were printed with exposure time 5 s, while printlets containing 12.50%, 20.00%, and 27.50% were printed with exposure time 10 s because it was not possible to print more than 1 printlet with exposure time 5 s. All printlets were fabricated without bottom layers, and with layer thickness 0.1 mm.
Determination of mass, dimension and tensile strength of printlets
Mass was determined on 20 printlets, and dimension (digital caliper, Vogel, Germany) was determined on 10 printlets for each formulation. Tensile strength of all formulations was calculated according to the following equation [3]:
σx=2F/πDt
Where:
σx is the tensile strength; F is the tablet breaking force (load); D and t are the diameter and thickness of printlets, respectively.
In vitro drug release testing
Atomoxetine dissolution rate from 3D printlets was tested using USP IV (Flow-through cell, CE7 smart, Sotax, Switzerland) apparatus. Three printlets of each formulation were tested in 250 ml of distilled water at 37±0.5 °C, with a flow rate of 8 ml per minute during 8 h. The amount of dissolved atomoxetine was determined by UV/VIS spectrophotometry at 270 nm (Evolution 300, Thermo Fisher Scientific, Cambridge).
RESULTS AND DISCUSSION
3D printing process
Printlets containing four different amounts of atomoxetine were successfully produced using photoreactive dispersions by the DLP printer. Achieved doses of atomoxetine in printlets were 5.84±0.54 mg, 20.24±0.82 mg, 32.46±1.69 mg and 58.08±3.09 mg, which is a wide range of doses that allow personalization of therapy. Also, total printing time for 10 printlets was 5 and 7 minutes, for exposition time 5 s and 10 s, respectively, which is significantly shorter than printing time in other 3D printing technologies.
Mass, dimension and tensile strength of printlets
Mass, diameter and thickness are shown in Table 2, while tensile strengths of all formulations are shown in Figure 1.
The increase in the atomoxetine content led to the fabrication of printlets with a higher mass and dimensions, due to the higher proportion of atomoxetine particles that were not dissolved in photoreactive mixture and their scattering phenomena in the light beam.
Increasing content of active ingredient led to higher tensile strength of printlets, and all formulations had tensile strength around 1 MPa, which can be sufficient for small batches [4].
Dissolution profiles
Dissolution profiles of formulations containing different content of atomoxetine are shown in Figure 2. Only from formulation A1 more than 80% of atomoxetine was released after 2 h, which can be a consequence of shorter exposition time set during the printing for this formulation, while formulations A2-A4 overlapped during the first hour of the test and achieved sustained release during 8h. After 8h, 88.94%, 79.77%, 77.53% and 72.54% of atomoxetine were released from formulations A1, A2, A3, and A4, respectively.
CONCLUSION
The possibility of successful 3D DLP printing of the printlets using the active ingredient dispersed in the photopolymer mixture, with optimization of printing process parameters for rapid printlet production, has been demonstrated. Printlets with higher content of dispersed atomoxetine have shown decreased drug release rate after 8h, with increasing tensile strength, mass, and dimensions, due to interactions with the light beam.
PB  - International Association for Pharmaceutical Technology, Mainz, Germany
C3  - 12th World Meeting on Pharmaceutics, Biopharmaceutics and Pharmaceutical Technology, 11-14 May 2021, Vienna, Austria, Virtual meeting
T1  - Characterization of printlets obtained from photoreactive dispersions by digital light processing (DLP) 3D technology
SP  - 1
EP  - 2
UR  - https://hdl.handle.net/21.15107/rcub_farfar_5325
ER  - 

@conference{
author = "Krkobabić, Mirjana and Pešić, Nikola and Boljević, Gordana and Medarević, Đorđe and Ibrić, Svetlana",
year = "2021",
abstract = "INTRODUCTION
Application of the 3D printing in pharmacy make possible production of small batches of solid dosage forms for oral administration (printlets) with different dose and release characteristics that can be customized to specific patient needs [1]. Digital light processing (DLP), one type of 3D printing technology, is based on a UV-triggered localized photopolymerization process of liquid resins [2]. The aim of this study was 3D printing from photoreactive dispersions with different amounts of solid phase and characterization of obtained printlets.
MATERIALS
Different photoreactive dispersions were prepared from poly(ethylene glycol) diacrylate 700 (PEGDA 700, Sigma-Aldrich, Japan), poly(ethylene glycol) 400 (PEG 400, Fagron, Netherlands), atomoxetine (kindly provided by Hemofarm AD, Vrsac, Serbia), diphenyl(2,4,6-trimethylbenzoyl) phosphine oxide (DPPO, Sigma-Aldrich, Germany).
Preparation of photoreactive dispersions
Atomoxetine was used as an active ingredient, while PEGDA was used as a photopolymer and DPPO as a photoinitiator in photoreactive dispersions. PEG 400 was used as an excipient to overcome very slow and incomplete drug release from printlets fabricated by photopolymerization using DLP technology. The ratio of PEGDA and PEG 400 was constant in all formulations (3:1), and content of atomoxetine was varied from 5% to 27.5% (Table 1). 30 g of each formulation was prepared by mixing on the magnetic stirrer for 15 minutes, protected from the light.
3D printing of atomoxetine printlets
The templates used for printlets were designed by Autodesk Fusion 360 software and exported as a stereolithography file (.stl) into Creation Workshop X 1.2.1 software. All printlets were fabricated using DLP printer Duplicator 7 (Wanhao, Zhejiang, China). The selected shape was cylinder (8 mm diameter and 2 mm height). Printlets containing 5.00% of atomoxetine were printed with exposure time 5 s, while printlets containing 12.50%, 20.00%, and 27.50% were printed with exposure time 10 s because it was not possible to print more than 1 printlet with exposure time 5 s. All printlets were fabricated without bottom layers, and with layer thickness 0.1 mm.
Determination of mass, dimension and tensile strength of printlets
Mass was determined on 20 printlets, and dimension (digital caliper, Vogel, Germany) was determined on 10 printlets for each formulation. Tensile strength of all formulations was calculated according to the following equation [3]:
σx=2F/πDt
Where:
σx is the tensile strength; F is the tablet breaking force (load); D and t are the diameter and thickness of printlets, respectively.
In vitro drug release testing
Atomoxetine dissolution rate from 3D printlets was tested using USP IV (Flow-through cell, CE7 smart, Sotax, Switzerland) apparatus. Three printlets of each formulation were tested in 250 ml of distilled water at 37±0.5 °C, with a flow rate of 8 ml per minute during 8 h. The amount of dissolved atomoxetine was determined by UV/VIS spectrophotometry at 270 nm (Evolution 300, Thermo Fisher Scientific, Cambridge).
RESULTS AND DISCUSSION
3D printing process
Printlets containing four different amounts of atomoxetine were successfully produced using photoreactive dispersions by the DLP printer. Achieved doses of atomoxetine in printlets were 5.84±0.54 mg, 20.24±0.82 mg, 32.46±1.69 mg and 58.08±3.09 mg, which is a wide range of doses that allow personalization of therapy. Also, total printing time for 10 printlets was 5 and 7 minutes, for exposition time 5 s and 10 s, respectively, which is significantly shorter than printing time in other 3D printing technologies.
Mass, dimension and tensile strength of printlets
Mass, diameter and thickness are shown in Table 2, while tensile strengths of all formulations are shown in Figure 1.
The increase in the atomoxetine content led to the fabrication of printlets with a higher mass and dimensions, due to the higher proportion of atomoxetine particles that were not dissolved in photoreactive mixture and their scattering phenomena in the light beam.
Increasing content of active ingredient led to higher tensile strength of printlets, and all formulations had tensile strength around 1 MPa, which can be sufficient for small batches [4].
Dissolution profiles
Dissolution profiles of formulations containing different content of atomoxetine are shown in Figure 2. Only from formulation A1 more than 80% of atomoxetine was released after 2 h, which can be a consequence of shorter exposition time set during the printing for this formulation, while formulations A2-A4 overlapped during the first hour of the test and achieved sustained release during 8h. After 8h, 88.94%, 79.77%, 77.53% and 72.54% of atomoxetine were released from formulations A1, A2, A3, and A4, respectively.
CONCLUSION
The possibility of successful 3D DLP printing of the printlets using the active ingredient dispersed in the photopolymer mixture, with optimization of printing process parameters for rapid printlet production, has been demonstrated. Printlets with higher content of dispersed atomoxetine have shown decreased drug release rate after 8h, with increasing tensile strength, mass, and dimensions, due to interactions with the light beam.",
publisher = "International Association for Pharmaceutical Technology, Mainz, Germany",
journal = "12th World Meeting on Pharmaceutics, Biopharmaceutics and Pharmaceutical Technology, 11-14 May 2021, Vienna, Austria, Virtual meeting",
title = "Characterization of printlets obtained from photoreactive dispersions by digital light processing (DLP) 3D technology",
pages = "1-2",
url = "https://hdl.handle.net/21.15107/rcub_farfar_5325"
}

Krkobabić, M., Pešić, N., Boljević, G., Medarević, Đ.,& Ibrić, S.. (2021). Characterization of printlets obtained from photoreactive dispersions by digital light processing (DLP) 3D technology. in 12th World Meeting on Pharmaceutics, Biopharmaceutics and Pharmaceutical Technology, 11-14 May 2021, Vienna, Austria, Virtual meeting
International Association for Pharmaceutical Technology, Mainz, Germany., 1-2.
https://hdl.handle.net/21.15107/rcub_farfar_5325

Krkobabić M, Pešić N, Boljević G, Medarević Đ, Ibrić S. Characterization of printlets obtained from photoreactive dispersions by digital light processing (DLP) 3D technology. in 12th World Meeting on Pharmaceutics, Biopharmaceutics and Pharmaceutical Technology, 11-14 May 2021, Vienna, Austria, Virtual meeting. 2021;:1-2.
https://hdl.handle.net/21.15107/rcub_farfar_5325 .

Krkobabić, Mirjana, Pešić, Nikola, Boljević, Gordana, Medarević, Đorđe, Ibrić, Svetlana, "Characterization of printlets obtained from photoreactive dispersions by digital light processing (DLP) 3D technology" in 12th World Meeting on Pharmaceutics, Biopharmaceutics and Pharmaceutical Technology, 11-14 May 2021, Vienna, Austria, Virtual meeting (2021):1-2,
https://hdl.handle.net/21.15107/rcub_farfar_5325 .

TY  - JOUR
AU  - Pešić, Nikola
AU  - Dapčević, Aleksandra
AU  - Ivković, Branka
AU  - Kachrimanis, Kyriakos
AU  - Mitrić, Miodrag
AU  - Ibrić, Svetlana
AU  - Medarević, Đorđe
PY  - 2021
UR  - https://farfar.pharmacy.bg.ac.rs/handle/123456789/3964
AB  - In this study, four low molecular weight (LMW) excipients, tryptophan (TRY), phenylalanine (PHE), lysine (LYS) and saccharin (SAC) were evaluated as co-formers to generate co-amorphous systems (CAMS) by ball milling with carvedilol (CRV). Mixtures of CRV and LMW excipient in 1:0.5, 1:1 and 1:2 drug:excipient molar ratios were ball milled and analysed by powder X-ray diffraction (PXRD), differential scanning calorimetry (DSC), Fourier transform (FT-IR) infrared spectroscopy and dissolution testing. CAMS were formed by milling of a mixture of CRV with TRY in 1:2 M ratio and SAC in 1:1 M ratio, while amorphization of only CRV was achieved in other mixtures with SAC. In other samples containing TRY and PHE, milling resulted in partial amorphization, while LYS was the least suitable excipient for the amorphization of CRV. Unexpectedly, the highest supersaturation of CRV was achieved from samples containing CRV and LYS in 1:1 and 1:2 M ratios, despite the absence of a significant reduction in CRV crystallinity upon milling of these samples. Increase of hydrophobic surface area caused by milling of samples with TRY and PHE and agglomeration during dissolution testing of samples containing SAC are likely causes of poor dissolution performance of mixtures containing fully or partially amorphous CRV.
PB  - Elsevier B.V.
T2  - International Journal of Pharmaceutics
T1  - Potential application of low molecular weight excipients for amorphization and dissolution enhancement of carvedilol
VL  - 608
DO  - 10.1016/j.ijpharm.2021.121033
ER  - 

@article{
author = "Pešić, Nikola and Dapčević, Aleksandra and Ivković, Branka and Kachrimanis, Kyriakos and Mitrić, Miodrag and Ibrić, Svetlana and Medarević, Đorđe",
year = "2021",
abstract = "In this study, four low molecular weight (LMW) excipients, tryptophan (TRY), phenylalanine (PHE), lysine (LYS) and saccharin (SAC) were evaluated as co-formers to generate co-amorphous systems (CAMS) by ball milling with carvedilol (CRV). Mixtures of CRV and LMW excipient in 1:0.5, 1:1 and 1:2 drug:excipient molar ratios were ball milled and analysed by powder X-ray diffraction (PXRD), differential scanning calorimetry (DSC), Fourier transform (FT-IR) infrared spectroscopy and dissolution testing. CAMS were formed by milling of a mixture of CRV with TRY in 1:2 M ratio and SAC in 1:1 M ratio, while amorphization of only CRV was achieved in other mixtures with SAC. In other samples containing TRY and PHE, milling resulted in partial amorphization, while LYS was the least suitable excipient for the amorphization of CRV. Unexpectedly, the highest supersaturation of CRV was achieved from samples containing CRV and LYS in 1:1 and 1:2 M ratios, despite the absence of a significant reduction in CRV crystallinity upon milling of these samples. Increase of hydrophobic surface area caused by milling of samples with TRY and PHE and agglomeration during dissolution testing of samples containing SAC are likely causes of poor dissolution performance of mixtures containing fully or partially amorphous CRV.",
publisher = "Elsevier B.V.",
journal = "International Journal of Pharmaceutics",
title = "Potential application of low molecular weight excipients for amorphization and dissolution enhancement of carvedilol",
volume = "608",
doi = "10.1016/j.ijpharm.2021.121033"
}

Pešić, N., Dapčević, A., Ivković, B., Kachrimanis, K., Mitrić, M., Ibrić, S.,& Medarević, Đ.. (2021). Potential application of low molecular weight excipients for amorphization and dissolution enhancement of carvedilol. in International Journal of Pharmaceutics
Elsevier B.V.., 608.
https://doi.org/10.1016/j.ijpharm.2021.121033

Pešić N, Dapčević A, Ivković B, Kachrimanis K, Mitrić M, Ibrić S, Medarević Đ. Potential application of low molecular weight excipients for amorphization and dissolution enhancement of carvedilol. in International Journal of Pharmaceutics. 2021;608.
doi:10.1016/j.ijpharm.2021.121033 .

Pešić, Nikola, Dapčević, Aleksandra, Ivković, Branka, Kachrimanis, Kyriakos, Mitrić, Miodrag, Ibrić, Svetlana, Medarević, Đorđe, "Potential application of low molecular weight excipients for amorphization and dissolution enhancement of carvedilol" in International Journal of Pharmaceutics, 608 (2021),
https://doi.org/10.1016/j.ijpharm.2021.121033 . .

TY  - JOUR
AU  - Milovanović, Stoja
AU  - Đuriš, Jelena
AU  - Dapčević, Aleksandra
AU  - Lučić-Škorić, Marija
AU  - Medarević, Đorđe
AU  - Pavlović, Stefan
AU  - Ibrić, Svetlana
PY  - 2021
UR  - https://farfar.pharmacy.bg.ac.rs/handle/123456789/3782
AB  - This study investigates pharmaceutical polymers (Soluplus®, HPMCAS, and Eudragit® E100) and supercritical CO2-assisted process for preparation of floating valsartan delivery systems. Tested process (at pressure of 30 MPa and temperature of 100 °C during 2 h) enabled preparation of stable porous valsartan formulations which was confirmed with FESEM and mercury intrusion porosimetry analysis. The bulk density of obtained formulations was lower than 550 kg/m3. FTIR, DSC, and PXRD analysis indicated that there was no chemical interaction between the drug and polymers and that amorphous solid dispersions were obtained. Formulations with Soluplus® and HPMCAS retained its buoyancy in 0.1 M HCl for longer than 24 h, while formulation with Eudragit® E100 retained its buoyancy up to 2 h. Controlled valsartan release was influenced by solubility of polymers in the tested release medium, which was confirmed by UV/VIS spectroscopy. The obtained results provided framework for further development of floating drug delivery system using an environmental friendly process.
PB  - Springer Science and Business Media B.V.
T2  - Journal of Polymer Research
T1  - Preparation of floating polymer-valsartan delivery systems using supercritical CO2
VL  - 28
IS  - 3
DO  - 10.1007/s10965-021-02440-1
ER  - 

@article{
author = "Milovanović, Stoja and Đuriš, Jelena and Dapčević, Aleksandra and Lučić-Škorić, Marija and Medarević, Đorđe and Pavlović, Stefan and Ibrić, Svetlana",
year = "2021",
abstract = "This study investigates pharmaceutical polymers (Soluplus®, HPMCAS, and Eudragit® E100) and supercritical CO2-assisted process for preparation of floating valsartan delivery systems. Tested process (at pressure of 30 MPa and temperature of 100 °C during 2 h) enabled preparation of stable porous valsartan formulations which was confirmed with FESEM and mercury intrusion porosimetry analysis. The bulk density of obtained formulations was lower than 550 kg/m3. FTIR, DSC, and PXRD analysis indicated that there was no chemical interaction between the drug and polymers and that amorphous solid dispersions were obtained. Formulations with Soluplus® and HPMCAS retained its buoyancy in 0.1 M HCl for longer than 24 h, while formulation with Eudragit® E100 retained its buoyancy up to 2 h. Controlled valsartan release was influenced by solubility of polymers in the tested release medium, which was confirmed by UV/VIS spectroscopy. The obtained results provided framework for further development of floating drug delivery system using an environmental friendly process.",
publisher = "Springer Science and Business Media B.V.",
journal = "Journal of Polymer Research",
title = "Preparation of floating polymer-valsartan delivery systems using supercritical CO2",
volume = "28",
number = "3",
doi = "10.1007/s10965-021-02440-1"
}

Milovanović, S., Đuriš, J., Dapčević, A., Lučić-Škorić, M., Medarević, Đ., Pavlović, S.,& Ibrić, S.. (2021). Preparation of floating polymer-valsartan delivery systems using supercritical CO2. in Journal of Polymer Research
Springer Science and Business Media B.V.., 28(3).
https://doi.org/10.1007/s10965-021-02440-1

Milovanović S, Đuriš J, Dapčević A, Lučić-Škorić M, Medarević Đ, Pavlović S, Ibrić S. Preparation of floating polymer-valsartan delivery systems using supercritical CO2. in Journal of Polymer Research. 2021;28(3).
doi:10.1007/s10965-021-02440-1 .

Milovanović, Stoja, Đuriš, Jelena, Dapčević, Aleksandra, Lučić-Škorić, Marija, Medarević, Đorđe, Pavlović, Stefan, Ibrić, Svetlana, "Preparation of floating polymer-valsartan delivery systems using supercritical CO2" in Journal of Polymer Research, 28, no. 3 (2021),
https://doi.org/10.1007/s10965-021-02440-1 . .

TY  - JOUR
AU  - Medarević, Đorđe
AU  - Đuriš, Jelena
AU  - Krkobabić, Mirjana
AU  - Ibrić, Svetlana
PY  - 2021
UR  - https://farfar.pharmacy.bg.ac.rs/handle/123456789/4013
AB  - Co-processing is commonly used approach to improve functional characteristics of pharmaceutical excipients to become suitable for tablet production by direct compression. This study aimed to improve tableting characteristics of lactose monohydrate (LMH) by co-processing by fluid-bed melt granulation with addition of hydrophilic (PEG 4000 and poloxamer 188) and lipophilic (glyceryl palmitostearate) meltable binders. In addition to binding purpose, hydrophilic and lipophilic excipients were added to achieve self-lubricating properties of mixture. Co-processed mixtures exhibit superior flow properties compared to pure LMH and comparable or better flowability relative to commercial excipient Ludipress®. Compaction of mixtures co-processed with 20% PEG 4000 and 20% poloxamer 188 resulted in tablets with acceptable tensile strength (>2 MPa) and good lubricating properties (ejection and detachment stress values below 5 MPa) in a wide range of compression pressures. While the best lubricating properties were observed when glyceryl palmitostearate was used as meltable binder, obtained tablets failed to fulfil required mechanical characteristics. Although addition of meltable binder improves interparticle bonding, disintegration time was not prolonged compared to commercial excipient Ludipress®. Co-processed mixtures containing 20% of either PEG 4000 or poloxamer 188 showed superior tabletability and lubricant properties relative to LMH and Ludipress® and can be good candidates for tablet production by direct compression.
PB  - MDPI
T2  - Pharmaceutics
T1  - Improving tableting performance of lactose monohydrate by fluid-bed melt granulation co-processing
VL  - 13
IS  - 12
DO  - 10.3390/pharmaceutics13122165
ER  - 

@article{
author = "Medarević, Đorđe and Đuriš, Jelena and Krkobabić, Mirjana and Ibrić, Svetlana",
year = "2021",
abstract = "Co-processing is commonly used approach to improve functional characteristics of pharmaceutical excipients to become suitable for tablet production by direct compression. This study aimed to improve tableting characteristics of lactose monohydrate (LMH) by co-processing by fluid-bed melt granulation with addition of hydrophilic (PEG 4000 and poloxamer 188) and lipophilic (glyceryl palmitostearate) meltable binders. In addition to binding purpose, hydrophilic and lipophilic excipients were added to achieve self-lubricating properties of mixture. Co-processed mixtures exhibit superior flow properties compared to pure LMH and comparable or better flowability relative to commercial excipient Ludipress®. Compaction of mixtures co-processed with 20% PEG 4000 and 20% poloxamer 188 resulted in tablets with acceptable tensile strength (>2 MPa) and good lubricating properties (ejection and detachment stress values below 5 MPa) in a wide range of compression pressures. While the best lubricating properties were observed when glyceryl palmitostearate was used as meltable binder, obtained tablets failed to fulfil required mechanical characteristics. Although addition of meltable binder improves interparticle bonding, disintegration time was not prolonged compared to commercial excipient Ludipress®. Co-processed mixtures containing 20% of either PEG 4000 or poloxamer 188 showed superior tabletability and lubricant properties relative to LMH and Ludipress® and can be good candidates for tablet production by direct compression.",
publisher = "MDPI",
journal = "Pharmaceutics",
title = "Improving tableting performance of lactose monohydrate by fluid-bed melt granulation co-processing",
volume = "13",
number = "12",
doi = "10.3390/pharmaceutics13122165"
}

Medarević, Đ., Đuriš, J., Krkobabić, M.,& Ibrić, S.. (2021). Improving tableting performance of lactose monohydrate by fluid-bed melt granulation co-processing. in Pharmaceutics
MDPI., 13(12).
https://doi.org/10.3390/pharmaceutics13122165

Medarević Đ, Đuriš J, Krkobabić M, Ibrić S. Improving tableting performance of lactose monohydrate by fluid-bed melt granulation co-processing. in Pharmaceutics. 2021;13(12).
doi:10.3390/pharmaceutics13122165 .

Medarević, Đorđe, Đuriš, Jelena, Krkobabić, Mirjana, Ibrić, Svetlana, "Improving tableting performance of lactose monohydrate by fluid-bed melt granulation co-processing" in Pharmaceutics, 13, no. 12 (2021),
https://doi.org/10.3390/pharmaceutics13122165 . .

TY  - JOUR
AU  - Awad, Mahmoud E.
AU  - López-Galindo, Alberto
AU  - Medarević, Đorđe
AU  - Milenković, Marina
AU  - Ibrić, Svetlana
AU  - El-Rahmany, Mahmoud M.
AU  - Iborra, César
PY  - 2021
UR  - https://farfar.pharmacy.bg.ac.rs/handle/123456789/3800
AB  - The present research aims to enhance the antimicrobial activity of kaolinite surfaces by a one-step cost-effective and energy-efficient dry thermal reaction, producing an antibacterial and antifungal silver-kaolinite (Ag-Kao) nanocomposite agent. Pharmaceutical grade kaolin powder samples, with variable kaolinite structural order–disorder degree, were homogeneously mixed with silver nitrate in a proportion 1:4 AgNO3:kaolin (w/w) and sintered at 400 °C for 30 min. The composition, microstructure, microtexture and surface characteristics of the pyro-fabricated nanocomposites were characterized by XRD/XRF diffractometry, differential scanning calorimetry DSC, FT-IR spectroscopy, TEM/EDX, zeta potential (mV) measured within the 2–12 pH range, and BET method. Physicochemical stability was evaluated by silver dissociation testing under close-neutral and acidic conditions with Ag content assay using ICP-OES. The resulting Ag-Kao nanocomposites exhibited bulk silver contents ranging from 9.29% to 13.32% with high physicochemical stability in both neutral and acidic mediums (Ag dissociation rate <0.5% in 5 days). Ag nanocrystals exhibited particle sizes ranging from 5 to 30 nm, which were embedded and reinforced within the kaolinite matrix. The sizes of the Ag nanocrystals and their distribution patterns on the edges and faces of kaolinite platelets were controlled by the structural order–disorder degree. Highly ordered kaolinites (Hinckley Index, HI > 1) produced platelet edge-clustered silver nanocrystals due to the abundance of the dangling hydroxyls on platelet edges, while the highly disordered kaolinite (HI < 1) provided homogeneous platelet basal-doped silver nanocrystals due to the presence of some residual charges by exposed basal hydroxyl groups with interplatelet silver diffusivity. At pH 2, the magnitude of the positive surface charge was influenced by the silver nanocrystal size. Nanocomposites with the smallest silver nanocrystals (10–5 nm) exhibited the highest positive zeta potential (+15.2 mV to +17.0 mV), while those with larger silver nanocrystals (up to 30 nm) indicated lower positive zeta potential values (+9.5 mV to +3.6 mV). Under the same testing conditions using the Mueller-Hinton broth microdilution method, the raw kaolin samples did not show any significant antimicrobial activity, while all the pyro-fabricated Ag-Kao nanocomposite samples showed potent antibacterial and antifungal activity at low doses (MIC range 0.1–0.0125 mg/mL). Therefore, modulation of the effective electrostatic surface charge of the kaolinite platelets, via thermal doping of silver within their basal planes and edges, was found to be strongly dependent on the pH as well as the size and microtexture of the silver nanocrystals (mainly controlled by the order–disorder degree HI). The resulting modified nanostructure, with physicochemical stability and the efficient surface properties of the designed pyro-fabricated nanocomposite, led to an enhanced synergistic biophysical antimicrobial activity.
PB  - Elsevier B.V.
T2  - International Journal of Pharmaceutics
T1  - Enhanced antimicrobial activity and physicochemical stability of rapid pyro-fabricated silver-kaolinite nanocomposite
VL  - 598
DO  - 10.1016/j.ijpharm.2021.120372
ER  - 

@article{
author = "Awad, Mahmoud E. and López-Galindo, Alberto and Medarević, Đorđe and Milenković, Marina and Ibrić, Svetlana and El-Rahmany, Mahmoud M. and Iborra, César",
year = "2021",
abstract = "The present research aims to enhance the antimicrobial activity of kaolinite surfaces by a one-step cost-effective and energy-efficient dry thermal reaction, producing an antibacterial and antifungal silver-kaolinite (Ag-Kao) nanocomposite agent. Pharmaceutical grade kaolin powder samples, with variable kaolinite structural order–disorder degree, were homogeneously mixed with silver nitrate in a proportion 1:4 AgNO3:kaolin (w/w) and sintered at 400 °C for 30 min. The composition, microstructure, microtexture and surface characteristics of the pyro-fabricated nanocomposites were characterized by XRD/XRF diffractometry, differential scanning calorimetry DSC, FT-IR spectroscopy, TEM/EDX, zeta potential (mV) measured within the 2–12 pH range, and BET method. Physicochemical stability was evaluated by silver dissociation testing under close-neutral and acidic conditions with Ag content assay using ICP-OES. The resulting Ag-Kao nanocomposites exhibited bulk silver contents ranging from 9.29% to 13.32% with high physicochemical stability in both neutral and acidic mediums (Ag dissociation rate <0.5% in 5 days). Ag nanocrystals exhibited particle sizes ranging from 5 to 30 nm, which were embedded and reinforced within the kaolinite matrix. The sizes of the Ag nanocrystals and their distribution patterns on the edges and faces of kaolinite platelets were controlled by the structural order–disorder degree. Highly ordered kaolinites (Hinckley Index, HI > 1) produced platelet edge-clustered silver nanocrystals due to the abundance of the dangling hydroxyls on platelet edges, while the highly disordered kaolinite (HI < 1) provided homogeneous platelet basal-doped silver nanocrystals due to the presence of some residual charges by exposed basal hydroxyl groups with interplatelet silver diffusivity. At pH 2, the magnitude of the positive surface charge was influenced by the silver nanocrystal size. Nanocomposites with the smallest silver nanocrystals (10–5 nm) exhibited the highest positive zeta potential (+15.2 mV to +17.0 mV), while those with larger silver nanocrystals (up to 30 nm) indicated lower positive zeta potential values (+9.5 mV to +3.6 mV). Under the same testing conditions using the Mueller-Hinton broth microdilution method, the raw kaolin samples did not show any significant antimicrobial activity, while all the pyro-fabricated Ag-Kao nanocomposite samples showed potent antibacterial and antifungal activity at low doses (MIC range 0.1–0.0125 mg/mL). Therefore, modulation of the effective electrostatic surface charge of the kaolinite platelets, via thermal doping of silver within their basal planes and edges, was found to be strongly dependent on the pH as well as the size and microtexture of the silver nanocrystals (mainly controlled by the order–disorder degree HI). The resulting modified nanostructure, with physicochemical stability and the efficient surface properties of the designed pyro-fabricated nanocomposite, led to an enhanced synergistic biophysical antimicrobial activity.",
publisher = "Elsevier B.V.",
journal = "International Journal of Pharmaceutics",
title = "Enhanced antimicrobial activity and physicochemical stability of rapid pyro-fabricated silver-kaolinite nanocomposite",
volume = "598",
doi = "10.1016/j.ijpharm.2021.120372"
}

Awad, M. E., López-Galindo, A., Medarević, Đ., Milenković, M., Ibrić, S., El-Rahmany, M. M.,& Iborra, C.. (2021). Enhanced antimicrobial activity and physicochemical stability of rapid pyro-fabricated silver-kaolinite nanocomposite. in International Journal of Pharmaceutics
Elsevier B.V.., 598.
https://doi.org/10.1016/j.ijpharm.2021.120372

Awad ME, López-Galindo A, Medarević Đ, Milenković M, Ibrić S, El-Rahmany MM, Iborra C. Enhanced antimicrobial activity and physicochemical stability of rapid pyro-fabricated silver-kaolinite nanocomposite. in International Journal of Pharmaceutics. 2021;598.
doi:10.1016/j.ijpharm.2021.120372 .

Awad, Mahmoud E., López-Galindo, Alberto, Medarević, Đorđe, Milenković, Marina, Ibrić, Svetlana, El-Rahmany, Mahmoud M., Iborra, César, "Enhanced antimicrobial activity and physicochemical stability of rapid pyro-fabricated silver-kaolinite nanocomposite" in International Journal of Pharmaceutics, 598 (2021),
https://doi.org/10.1016/j.ijpharm.2021.120372 . .

TY  - JOUR
AU  - Đekić, Ljiljana
AU  - Čalija, Bojan
AU  - Medarević, Đorđe
PY  - 2020
UR  - https://farfar.pharmacy.bg.ac.rs/handle/123456789/3527
AB  - The study elucidated the combined effect of the formulation parameters (the relative contents of the copolymer (poloxamer 407 (P407)), the cosolvent (isopropyl alcohol), and the hydrophobic drug (ibuprofen)) on gelation, applicative properties, drug solubilization capacity and release kinetics of the P407 aqueous solutions under the common conditions of storage and topical administration. The presence of ibuprofen at a therapeutic concentration of 5% enhanced the increase in micellar volume fraction and allowed the gelation of the liquid solutions at P407 concentrations ≥ 15%. Light microscopy, DSC analysis, and rheological measurements pointed that P407 gels with 15–20% of the copolymer enabled controled precipitation of amorphous ibuprofen particles (≤100 μm) in perimicellar microchannels, while gels with 25–30% of P407 as well as increased relative content of the cosolvent in perimicellar aqueous phase, had capacity for complete ibuprofen solubilization. The dissolution of the drug particles during the in vitro drug release test, maintained the drug concentration gradient between the perimicellar microchannels and the acceptor medium allowing diffusion-based sustained drug release up to 12 h. The gels with completely solubilized drug notably decrease drug release rate and the cumulative amount of the drug released. Harmonization of the investigated formulation parameters was critical to the formulation of P407 gels that could be promising drug delivery systems for sustained percutaneous delivery of the hydrophobic model drug ibuprofen with reduced frequency of administration and improved patient compliance.
PB  - Elsevier B.V.
T2  - Journal of Molecular Liquids
T1  - Gelation behavior, drug solubilization capacity and release kinetics of poloxamer 407 aqueous solutions: The combined effect of copolymer, cosolvent and hydrophobic drug
VL  - 303
DO  - 10.1016/j.molliq.2020.112639
ER  - 

@article{
author = "Đekić, Ljiljana and Čalija, Bojan and Medarević, Đorđe",
year = "2020",
abstract = "The study elucidated the combined effect of the formulation parameters (the relative contents of the copolymer (poloxamer 407 (P407)), the cosolvent (isopropyl alcohol), and the hydrophobic drug (ibuprofen)) on gelation, applicative properties, drug solubilization capacity and release kinetics of the P407 aqueous solutions under the common conditions of storage and topical administration. The presence of ibuprofen at a therapeutic concentration of 5% enhanced the increase in micellar volume fraction and allowed the gelation of the liquid solutions at P407 concentrations ≥ 15%. Light microscopy, DSC analysis, and rheological measurements pointed that P407 gels with 15–20% of the copolymer enabled controled precipitation of amorphous ibuprofen particles (≤100 μm) in perimicellar microchannels, while gels with 25–30% of P407 as well as increased relative content of the cosolvent in perimicellar aqueous phase, had capacity for complete ibuprofen solubilization. The dissolution of the drug particles during the in vitro drug release test, maintained the drug concentration gradient between the perimicellar microchannels and the acceptor medium allowing diffusion-based sustained drug release up to 12 h. The gels with completely solubilized drug notably decrease drug release rate and the cumulative amount of the drug released. Harmonization of the investigated formulation parameters was critical to the formulation of P407 gels that could be promising drug delivery systems for sustained percutaneous delivery of the hydrophobic model drug ibuprofen with reduced frequency of administration and improved patient compliance.",
publisher = "Elsevier B.V.",
journal = "Journal of Molecular Liquids",
title = "Gelation behavior, drug solubilization capacity and release kinetics of poloxamer 407 aqueous solutions: The combined effect of copolymer, cosolvent and hydrophobic drug",
volume = "303",
doi = "10.1016/j.molliq.2020.112639"
}

Đekić, L., Čalija, B.,& Medarević, Đ.. (2020). Gelation behavior, drug solubilization capacity and release kinetics of poloxamer 407 aqueous solutions: The combined effect of copolymer, cosolvent and hydrophobic drug. in Journal of Molecular Liquids
Elsevier B.V.., 303.
https://doi.org/10.1016/j.molliq.2020.112639

Đekić L, Čalija B, Medarević Đ. Gelation behavior, drug solubilization capacity and release kinetics of poloxamer 407 aqueous solutions: The combined effect of copolymer, cosolvent and hydrophobic drug. in Journal of Molecular Liquids. 2020;303.
doi:10.1016/j.molliq.2020.112639 .

Đekić, Ljiljana, Čalija, Bojan, Medarević, Đorđe, "Gelation behavior, drug solubilization capacity and release kinetics of poloxamer 407 aqueous solutions: The combined effect of copolymer, cosolvent and hydrophobic drug" in Journal of Molecular Liquids, 303 (2020),
https://doi.org/10.1016/j.molliq.2020.112639 . .