TY  - JOUR
AU  - Gáborová, Mária
AU  - Vágvölgyi, Máté
AU  - Tayeb, Bizhar Ahmed
AU  - Minorics, Renáta
AU  - Zupkó, István
AU  - Jurček, Ondřej
AU  - Béni, Szabolcs
AU  - Kubínová, Renata
AU  - Balogh, György Tibor
AU  - Hunyadi, Attila
TI  - Diterpenes Isolated from Three Different Plectranthus Sensu Lato Species and Their Antiproliferative Activities against Gynecological and Glioblastoma Cancer Cells
JF  - ACS OMEGA
J2  - ACS OMEGA
PY  - 2024
SN  - 2470-1343
DO  - 10.1021/acsomega.4c00800
UR  - https://m2.mtmt.hu/api/publication/34779108
ID  - 34779108
LA  - English
DB  - MTMT
ER  - 

TY  - JOUR
AU  - Csorba, Anita
AU  - Katona, Gábor
AU  - Budai-Szűcs, Mária
AU  - Balogh Weiser, Diána
AU  - Molnár, P.
AU  - Maka, Erika
AU  - Nochta-Kazsoki, Adrienn Katalin
AU  - Vajna, Márton Antal
AU  - Zelkó, Romána
AU  - Nagy, Zoltán Zsolt
AU  - Balogh, György Tibor
TI  - A Comparative Pharmacokinetic Study for Cysteamine-Containing Eye Drops as an Orphan Topical Therapy in Cystinosis
JF  - INTERNATIONAL JOURNAL OF MOLECULAR SCIENCES
J2  - INT J MOL SCI
VL  - 25
PY  - 2024
IS  - 3
PG  - 14
SN  - 1661-6596
DO  - 10.3390/ijms25031623
UR  - https://m2.mtmt.hu/api/publication/34538437
ID  - 34538437
N1  - Department of Ophthalmology, Semmelweis University, Mária Street 39, Budapest, H-1085, Hungary            
            Institute of Pharmaceutical Technology and Regulatory Affairs, Faculty of Pharmacy, University of Szeged, Eötvös Street 6, Szeged, H-6720, Hungary            
            Department of Physical Chemistry and Materials Science, Faculty of Chemical Technology and Biotechnology, Budapest University of Technology and Economics, Műegyetem rkp. 3, Budapest, H-1111, Hungary            
            Molteam Llc., Mélyfúró Street 4, Budapest, H-1151, Hungary            
            University Pharmacy Department of Pharmacy Administration, Semmelweis University, Hőgyes Endre Street 7-9, Budapest, H-1092, Hungary            
            Department of Pharmaceutical Chemistry, Semmelweis University, Hőgyes Endre Street 7-9, Budapest, H-1092, Hungary            
            Export Date: 23 February 2024            
            Correspondence Address: Csorba, A.; Department of Ophthalmology, Mária Street 39, Hungary; email: csorba.anita@semmelweis-univ.hu            
            Correspondence Address: Balogh, G.T.; Department of Pharmaceutical Chemistry, Hőgyes Endre Street 7-9, Hungary; email: balogh.gyorgy.tibor@semmelweis.hu
LA  - English
DB  - MTMT
ER  - 

TY  - JOUR
AU  - Safaa, Mohammed Omer
AU  - Nagy, Nándor
AU  - Szőcs, Emőke
AU  - Kádár, Szabina
AU  - Völgyi, Gergely
AU  - Pinke, Balázs
AU  - Mészáros, László
AU  - Katona, Gábor
AU  - Vincze, Anna
AU  - Dormán, Péter
AU  - Nagy, Zoltán Zsolt
AU  - Balogh, György Tibor
AU  - Nochta-Kazsoki, Adrienn Katalin
AU  - Zelkó, Romána
TI  - Development of innovative electrospun nepafenac-loaded nanofibers-based ophthalmic inserts
JF  - INTERNATIONAL JOURNAL OF PHARMACEUTICS
J2  - INT J PHARM
VL  - 647
PY  - 2023
PG  - 13
SN  - 0378-5173
DO  - 10.1016/j.ijpharm.2023.123554
UR  - https://m2.mtmt.hu/api/publication/34225112
ID  - 34225112
N1  - University Pharmacy Department of Pharmacy Administration, Semmelweis University, Hőgyes Endre Street 7-9, Budapest, H-1092, Hungary            
            Department of Anatomy, Histology and Embryology Semmelweis University, Tűzoltó Street 58, Budapest, H-1094, Hungary            
            Department of Organic Chemistry and Technology, Faculty of Chemical Technology and Biotechnology, Budapest University of Technology and Economics, Műegyetem Rkp. 3, Budapest, H-1111, Hungary            
            Department of Pharmaceutical Chemistry, Semmelweis University, Hőgyes Endre Street 9, Budapest, H-1092, Hungary            
            Department of Polymer Engineering, Faculty of Mechanical Engineering, Budapest University of Technology and Economics, Műegyetem Rkp. 3, Budapest, H-1111, Hungary            
            Institute of Pharmaceutical Technology and Regulatory Affairs, University of Szeged, Eötvös u. 6, Szeged, H-6720, Hungary            
            Department of Chemical and Environmental Process Engineering, Budapest University of Technology and Economics, Műegyetem Rkp. 3, Budapest, H-1111, Hungary            
            Department of Ophthalmology, Semmelweis University, Ma ́ria Street 39, Budapest, 1085, Hungary            
            Export Date: 1 March 2024            
            CODEN: IJPHD            
            Correspondence Address: Kazsoki, A.; University Pharmacy Department of Pharmacy Administration, Hőgyes Endre Street 7-9, Hungary; email: kazsoki.adrienn@semmelweis.hu            
            Chemicals/CAS: 2 hydroxypropyl beta cyclodextrin, 94035-02-6, 128446-35-5; nepafenac, 78281-72-8; poloxamer, 9003-11-6; polyvinyl alcohol, 37380-95-3, 9002-89-5            
            Tradenames: nevanac            
            Manufacturers: TCI, Japan
LA  - English
DB  - MTMT
ER  - 

TY  - CONF
AU  - Vincze, Anna
AU  - Balogh, György Tibor
TI  - In vitro and ex vivo test systems in the development of cyclodextrin-enabled eye drops
T2  - EUROCD 2023 7th European Cyclodextrin Conference
PY  - 2023
UR  - https://m2.mtmt.hu/api/publication/34165281
ID  - 34165281
LA  - English
DB  - MTMT
ER  - 

TY  - CONF
AU  - Erdős, Dóra
AU  - D. Marton, András
AU  - Balogh, György Tibor
TI  - Ginkgo biloba EGb 761® extract in vitro permeability study
T2  - EUROCD 2023 7th European Cyclodextrin Conference
PY  - 2023
UR  - https://m2.mtmt.hu/api/publication/34163444
ID  - 34163444
N1  - https://www.cyclodextrinconference.com/wp-content/uploads/2023/07/EuroCD-2023-Scientific-Program-5.pdf
LA  - English
DB  - MTMT
ER  - 

TY  - JOUR
AU  - Kovács, Ferenc
AU  - Huliák, Ildikó
AU  - Árva, Hédi
AU  - Csontné Kiricsi, Mónika
AU  - Erdős, Dóra
AU  - Kocsis, Marianna
AU  - Takács, Gergely
AU  - Balogh, György Tibor
AU  - Nagyné Frank, Éva
TI  - Medicinal Chemistry‐driven Approach to Novel 2‐Substituted Benzoxazole – Estradiol Chimeras: Synthesis, Anticancer Activity and Early ADME Profile
JF  - CHEMMEDCHEM
J2  - CHEMMEDCHEM
VL  - 18
PY  - 2023
IS  - 22
PG  - 9
SN  - 1860-7179
DO  - 10.1002/cmdc.202300352
UR  - https://m2.mtmt.hu/api/publication/34147665
ID  - 34147665
N1  - Department of Molecular and Analytical Chemistry, University of Szeged, Dóm tér 7–8, Szeged, 6720, Hungary            
            Department of Biochemistry and Molecular Biology, Doctoral School of Biology, University of Szeged, Közép fasor 52, Szeged, 6726, Hungary            
            Department of Chemical and Environmental Process Engineering, Budapest University of Technology and Economics, Műegyetem rkp. 3, Budapest, 1111, Hungary            
            Mcule.com Kft., Bartók Béla út 105–113, Budapest, 1115, Hungary            
            Department of Pharmaceutical Chemistry, Semmelweis University, Hőgyes E. 9, Budapest, 1085, Hungary            
            Export Date: 13 October 2023            
            CODEN: CHEMG            
            Correspondence Address: Frank, É.; Department of Molecular and Analytical Chemistry, Dóm tér 7–8, Hungary; email: frank@chem.u-szeged.hu            
            Correspondence Address: Balogh, G.T.; Department of Chemical and Environmental Process Engineering, Műegyetem rkp. 3, Hungary; email: balogh.gyorgy.tibor@semmelwies.hu
AB  - The efficient synthesis of novel estradiol‐based A‐ring‐fused oxazole derivatives, which can be considered as benzoxazole‐steroid domain‐integrated hybrids containing a common benzene structural motif, is described. The target compounds were prepared from steroidal 2‐aminophenol precursors by heterocycle formation or functional group interconversion (FGI) strategies. According to 2D projection‐based t‐distributed stochastic neighbor embedding (t‐SNE), the novel molecules were proved to represent a new chemical space among steroid drugs. They were characterized based on critical physicochemical parameters using in silico and experimental data. The performance of the compounds to inhibit cell proliferation was tested on four human cancer cell lines and non‐cancerous cells. Further examinations were performed to reveal IC50 and lipophilic ligand efficiency (LLE) values, cancer cell selectivity, and apoptosis‐triggering features. Pharmacological tests and LLE metric revealed that some derivatives, especially the 2‐(4‐ethylpiperazin‐1‐yl)oxazole derivative exhibit strong anticancer activity and trigger the apoptosis of cancer cells with relatively low promiscuity risk similarly to the structurally most closely‐related and intensively studied anticancer agent, 2‐methoxy‐estradiol.
LA  - English
DB  - MTMT
ER  - 

TY  - JOUR
AU  - Juhász, Ádám
AU  - Ungor, Ditta Anita
AU  - Varga, Norbert
AU  - Katona, Gábor
AU  - Balogh, György Tibor
AU  - Csapó, Edit
TI  - Lipid-Based Nanocarriers for Delivery of Neuroprotective Kynurenic Acid: Preparation, Characterization, and BBB Transport
JF  - INTERNATIONAL JOURNAL OF MOLECULAR SCIENCES
J2  - INT J MOL SCI
VL  - 24
PY  - 2023
IS  - 18
PG  - 13
SN  - 1661-6596
DO  - 10.3390/ijms241814251
UR  - https://m2.mtmt.hu/api/publication/34146936
ID  - 34146936
AB  - Encapsulation possibilities of an extensively investigated neuroprotective drug (kynurenic acid, KYNA) are studied via lipid-based nanocarriers to increase the blood–brain barrier (BBB) specific permeability. The outcomes of various preparation conditions such as stirring and sonication time, concentration of the lipid carriers and the drug, and the drug-to-lipid ratio are examined. Considering the experimentally determined encapsulation efficiency, hydrodynamic diameter, and ζ-potential values, the initial lipid and drug concentration as well as the stirring and sonication time of the preparation were optimized. The average hydrodynamic diameter of the prepared asolectin-(LIP) and water-soluble lipopolymer (WSLP)-based liposomes was found to be ca. 25 and 60 nm under physiological conditions. The physicochemical characterization of the colloidal carriers proves that the preparation of the drug-loaded liposomes was a successful process, and secondary interactions were indicated between the drug molecule and the polymer residues around the WSLP membrane. Dissolution profiles of the active molecule under physiological conditions were registered, and the release of the unformulated and encapsulated drug is very similar. In addition to this outcome, the in vitro polar brain lipid extract (porcine)-based permeability test proved the achievement of two- or fourfold higher BBB specific penetration and lipid membrane retention for KYNA in the liposomal carriers relative to the unformatted drug.
LA  - English
DB  - MTMT
ER  - 

TY  - JOUR
AU  - Takács, Gergely
AU  - Havasi, Dávid
AU  - Sándor, Márk
AU  - Dohánics, Zsolt
AU  - Balogh, György Tibor
AU  - Kiss, Róbert
TI  - DIY Virtual Chemical Libraries - Novel Starting Points for Drug Discovery
JF  - ACS MEDICINAL CHEMISTRY LETTERS
J2  - ACS MED CHEM LETT
VL  - 14
PY  - 2023
IS  - 9
SP  - 1188
EP  - 1197
PG  - 10
SN  - 1948-5875
DO  - 10.1021/acsmedchemlett.3c00146
UR  - https://m2.mtmt.hu/api/publication/34119941
ID  - 34119941
LA  - English
DB  - MTMT
ER  - 

TY  - JOUR
AU  - Tóth, Gergő D.
AU  - Kállai-Szabó, Nikolett
AU  - Lengyel, Miléna
AU  - Süvegh, Károly
AU  - Ender, Ferenc
AU  - Katona, Gábor
AU  - Nochta-Kazsoki, Adrienn Katalin
AU  - Zelkó, Romána
AU  - Antal, István
AU  - Balogh, György Tibor
AU  - Balogh Weiser, Diána
TI  - Nanoformulation of lipase from Porcine pancreas by electrospinning as a novel alternative for enzyme-based per os therapies
JF  - JOURNAL OF MOLECULAR LIQUIDS
J2  - J MOL LIQ
VL  - 389
PY  - 2023
PG  - 13
SN  - 0167-7322
DO  - 10.1016/j.molliq.2023.122819
UR  - https://m2.mtmt.hu/api/publication/34096036
ID  - 34096036
N1  - Department of Physical Chemistry and Materials Science, Budapest University of Technology and Economics, Műegyetem rkp. 3, Budapest, H-1111, Hungary            
            Department of Pharmaceutics, Semmelweis University, Hőgyes E. Street 7–9, Budapest, H-1092, Hungary            
            Eötvös Loránd University Laboratory of Nuclear Chemistry, P.O. Box 32, Budapest, H-1518, Hungary            
            Department of Electron Devices, Budapest University of Technology and Economics, Műegyetem rkp. 3, Budapest, H-1111, Hungary            
            Spinsplit Llc., Vend u. 17, Budapest, H-1025, Hungary            
            Institute of Pharmaceutical Technology and Regulatory Affairs, Faculty of Pharmacy, University of Szeged, Eötvös u. 6, Szeged, H-6720, Hungary            
            University Pharmacy, Department of Pharmacy Administration, Faculty of Pharmaceutical Sciences, Semmelweis University, Hőgyes E. Street 7–9, Budapest, H-1092, Hungary            
            Department of Pharmaceutical Chemistry, Faculty of Pharmaceutical Sciences, Semmelweis University, Hőgyes E. Street 7–9, Budapest, H-1092, Hungary            
            Department of Chemical and Environmental Process Engineering, Budapest University of Technology and Economics, Budapest, H-1111, Hungary            
            Department of Organic Chemistry and Technology, Budapest University of Technology and Economics, Műegyetem rkp. 3, Budapest, H-1111, Hungary            
            Export Date: 20 February 2024            
            CODEN: JMLID            
            Correspondence Address: Antal, I.; Department of Pharmaceutical Chemistry, Hőgyes E. Street 7–9, Hungary; email: antal.istvan@semmelweis.hu
LA  - English
DB  - MTMT
ER  - 

TY  - PAT
AU  - Balogh, György Tibor
AU  - Katona, Gábor
AU  - Csóka, Ildikó
AU  - Zupkó, István
AU  - Nagy, Zoltán Zsolt
AU  - Kiss, Huba
AU  - Takács, Ágnes
AU  - Csorba, Anita
TI  - Eye drop formulation. An ocular formulation comprising L-Ascorbic 6-palmitate (ASP) is provided. The formulation is useful in situation wherein the maintenance of corneal transparency is at risk e..g. during or after corneal surgeries
TS  - An ocular formulation comprising L-Ascorbic 6-palmitate (ASP) is provided. The formulation is useful in situation wherein the maintenance of corneal transparency is at risk e..g. during or after corneal surgeries
PY  - 2023
PG  - 30
UR  - https://m2.mtmt.hu/api/publication/34066167
ID  - 34066167
LA  - English
DB  - MTMT
ER  -