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Dive into the research topics where Dimitrios Stefanidis is active.

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Featured researches published by Dimitrios Stefanidis.


Antimicrobial Agents and Chemotherapy | 2014

Metabolism and Pharmacokinetics of the Anti-Hepatitis C Virus Nucleotide Prodrug GS-6620

Eisuke Murakami; Ting Wang; Darius Babusis; Eve-Irene Lepist; Dorothea Sauer; Yeojin Park; Jennifer E. Vela; Robert Shih; Gabriel Birkus; Dimitrios Stefanidis; Choung U. Kim; Aesop Cho; Adrian S. Ray

ABSTRACT The anti-hepatitis C virus nucleotide prodrug GS-6620 employs a double-prodrug approach, with l-alanine-isopropyl ester and phenol moieties attached to the 5′-phosphate that release the nucleoside monophosphate in hepatocytes and a 3′-isobutyryl ester added to improve permeability and oral bioavailability. Consistent with the stability found in intestinal homogenates, following oral administration, intact prodrug levels in blood plasma were the highest in dogs, followed by monkeys, and then were the lowest in hamsters. In contrast, liver levels of the triphosphate metabolite at the equivalent surface area-adjusted doses were highest in hamsters, followed by in dogs and monkeys. Studies in isolated primary hepatocytes suggest that relatively poor oral absorption in hamsters and monkeys was compensated for by relatively efficient hepatocyte activation. As intestinal absorption was found to be critical to the effectiveness of GS-6620 in nonclinical species, stomach pH, formulation, and food effect studies were completed in dogs. Consistent with in vitro absorption studies in Caco-2 cells, the absorption of GS-6620 was found to be complex and highly dependent on concentration. Higher rates of metabolism were observed at lower concentrations that were unable to saturate intestinal efflux transporters. In first-in-human clinical trials, the oral administration of GS-6620 resulted in poor plasma exposure relative to that observed in dogs and in large pharmacokinetic and pharmacodynamic variabilities. While a double-prodrug approach, including a 3′-isobutyryl ester, provided higher intrinsic intestinal permeability, this substitution appeared to be a metabolic liability, resulting in extensive intestinal metabolism and relatively poor oral absorption in humans.


Archive | 2014

Combination formulation of two antiviral compounds

Eric Gorman; Erik Mogalian; Reza Oliyai; Dimitrios Stefanidis; Lauren Wiser; Vahid Zia


Archive | 2012

Compositions and methods for treating hepatitis c virus

Darryl G. Cleary; Charles J. Reynolds; Miriam Michelle Berrey; Robert G. Hindes; William T. Symonds; Adrian S. Ray; Hongmei Mo; Christy M. Hebner; Reza Oliyai; Vahid Zia; Dimitrios Stefanidis; Rowchanak Pakdaman


Archive | 2014

Formulation of Syk inhibitors

Bei Li; Rowchanak Pakdaman; Diana Sperger; Dimitrios Stefanidis


Archive | 2014

SOLID DISPERSION FORMULATION OF AN ANTIVIRAL COMPOUND

Eric Gorman; Erik Mogalian; Reza Oliyai; Dimitrios Stefanidis; Vahid Zia


Archive | 2017

composições e métodos para o tratamento do vírus da hepatite c

Adrian S. Ray; Charles J. Reynolds; Christy M. Hebner; Darryl G. Cleary; Dimitrios Stefanidis; Hongmei Mo; Miriam Michelle Berrey; Reza Oliyai; Robert G. Hindes; Rowchanak Pakdaman; Vahid Zia; William T. Symonds


Archive | 2015

FORMULACIÓN EN DISPERSIÓN SÓLIDA DE UN COMPUESTO ANTIVIRAL

Reza Oliyai; Eric Gorman; Erik Mogalian; Dimitrios Stefanidis; Vahid Zia


Archive | 2015

FORMULACIÓN DE COMBINACIÓN DE DOS COMPUESTOS ANTIVIRALES

Eric Gorman; Reza Oliyai; Dimitrios Stefanidis; Lauren Wiser; Vahid Zia; Erik Mogalian


Archive | 2014

Formulation de combinaison de deux composés antiviraux

Ben Chal; Erik Mogalian; Rowchanak Pakdaman; Reza Oliyai; Dimitrios Stefanidis; Vahid Zia


Archive | 2014

Formulierung aus syk-hemmern

Bei Li; Diana Sperger; Dimitrios Stefanidis; Rowchanak Pakdaman

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Vahid Zia

Katholieke Universiteit Leuven

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Hongmei Mo

Queen Mary University of London

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