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1. Hepatitis C virus genetic diversity by geographic region within genotype 1-6 subtypes among patients treated with glecaprevir and pibrentasvir.

Author

Gretja Schnell, Preethi Krishnan, Rakesh Tripathi, Jill Beyer, Thomas Reisch, Michelle Irvin, Tatyana Dekhtyar, Liangjun Lu, Teresa I Ng, Wangang Xie, Tami Pilot-Matias, and Christine Collins

Subjects
Medicine, Science
Abstract

Hepatitis C virus (HCV) is genetically diverse and includes 7 genotypes and 67 confirmed subtypes, and the global distribution of each HCV genotype (GT) varies by geographic region. In this report, we utilized a large dataset of NS3/4A and NS5A sequences isolated from 2348 HCV GT1-6-infected patients treated with the regimen containing glecaprevir/pibrentasvir (GLE/PIB) to assess genetic diversity within HCV subtypes by geographic region using phylogenetic analyses, and evaluated the prevalence of baseline amino acid polymorphisms in NS3 and NS5A by region/country and phylogenetic cluster. Among 2348 NS3/4A and NS5A sequences, phylogenetic analysis identified 6 genotypes and 44 subtypes, including 3 GT1, 8 GT2, 3 GT3, 13 GT4, 1 GT5, and 16 GT6 subtypes. Phylogenetic analysis of HCV subtype 1a confirmed the presence of two clades, which differed by geographic region distribution and NS3 Q80K prevalence. We detected phylogenetic clustering by country in HCV subtypes 1a, 1b, 2a, 2b, and 5a, suggesting that genetically distinct virus lineages are circulating in different countries. In addition, two clades were detected in HCV GT4a and GT6e, and NS5A amino acid polymorphisms were differentially distributed between the 2 clades in each subtype. The prevalence of NS3 and NS5A baseline polymorphisms varied substantially by genotype and subtype; therefore, we also determined the activity of GLE or PIB against replicons containing NS3/4A or NS5A from HCV GT1-6 clinical samples representing 6 genotypes and 21 subtypes overall. GLE and PIB retained activity against the majority of HCV replicons containing NS3/4A or NS5A from HCV GT1-6 clinical samples, with a median EC50 of 0.29 nM for GLE and 1.1 pM for PIB in a transient replicon assay. The data presented in this report expands the available data on HCV epidemiology, subtype diversity by geographic region, and NS3 and NS5A baseline polymorphism prevalence.

Published
2018
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2. Resistance Analysis of a 3-Day Monotherapy Study with Glecaprevir or Pibrentasvir in Patients with Chronic Hepatitis C Virus Genotype 1 Infection

Author

Teresa I. Ng, Tami Pilot-Matias, Rakesh Tripathi, Gretja Schnell, Preethi Krishnan, Thomas Reisch, Jill Beyer, Tatyana Dekhtyar, Michelle Irvin, Liangjun Lu, Armen Asatryan, Andrew Campbell, Betty Yao, Sandra Lovell, Federico Mensa, Eric J. Lawitz, Jens Kort, and Christine Collins

Subjects
glecaprevir, pibrentasvir, monotherapy, resistance, HCV, ABT-493, ABT-530, Microbiology, QR1-502
Abstract

Glecaprevir (an NS3/4A protease inhibitor) and pibrentasvir (an NS5A inhibitor) are potent and pangenotypic hepatitis C virus (HCV) direct-acting antivirals. This report describes the baseline polymorphisms and treatment-emergent substitutions in NS3 or NS5A detected in samples from HCV genotype 1-infected patients receiving 3-day monotherapy of glecaprevir or pibrentasvir, respectively. None of the NS3 polymorphisms detected in the 47 baseline samples collected prior to glecaprevir monotherapy conferred reduced susceptibility to glecaprevir. The NS3 A156T substitution, which conferred resistance to glecaprevir but had low replication efficiency, emerged in one genotype 1a-infected patient among the 35 patients with available post-baseline sequence data. Baseline NS5A polymorphisms were detected in 12 of 40 patients prior to pibrentasvir monotherapy; most polymorphisms were single-position NS5A amino acid substitutions that did not confer resistance to pibrentasvir. Among the 19 patients with available post-baseline NS5A sequence data, 3 had treatment-emergent NS5A substitutions during pibrentasvir monotherapy. All treatment-emergent NS5A substitutions were linked multiple-position, almost exclusively double-position, substitutions that conferred resistance to pibrentasvir. Replicons engineered with these double-position substitutions had low replication efficiency. In conclusion, resistance-conferring substitutions emerged in a small number of genotype 1-infected patients during glecaprevir or pibrentasvir monotherapy; unlike other NS5A inhibitors, pibrentasvir did not select single-position NS5A substitutions during monotherapy.

Published
2018
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3. Characterization of demographics and NS5A genetic diversity for hepatitis C virus genotype 4-infected patients with or without cirrhosis treated with ombitasvir/paritaprevir/ritonavir

Author

Rakesh Tripathi, Tatyana Dekhtyar, Thomas Reisch, Coleen Hall, Tami Pilot-Matias, N. Mobashery, Yao Yu, Rebecca Redman, Christine Collins, Michelle Irvin, Gretja Schnell, Preethi Krishnan, and Jill Beyer

Subjects
Cyclopropanes, Male, 0301 basic medicine, Hepacivirus, Viral Nonstructural Proteins, medicine.disease_cause, 0302 clinical medicine, Genotype, Prevalence, Cluster Analysis, Anilides, Phylogeny, Aged, 80 and over, Molecular Epidemiology, Sulfonamides, virus diseases, Valine, Hepatitis C, Middle Aged, Europe, Treatment Outcome, Infectious Diseases, Female, 030211 gastroenterology & hepatology, Viral hepatitis, medicine.drug, Adult, Macrocyclic Compounds, Proline, Lactams, Macrocyclic, Hepatitis C virus, Biology, Antiviral Agents, 03 medical and health sciences, Clinical Trials, Phase II as Topic, Virology, Ombitasvir/paritaprevir/ritonavir, medicine, Humans, Aged, Demography, Ritonavir, Hepatology, Genetic Variation, Sequence Analysis, DNA, Hepatitis C, Chronic, medicine.disease, digestive system diseases, Ombitasvir, 030104 developmental biology, Clinical Trials, Phase III as Topic, Paritaprevir, North America, Carbamates
Abstract

Hepatitis C virus (HCV) genotype 4 (GT4) is genetically diverse with 17 confirmed and 4 provisional subtypes. In this report, HCV GT4-infected patient samples from Phase 2/3 clinical studies were analysed to characterize global demographics and genetic diversity of GT4 infection among patients treated with ombitasvir (OBV, NS5A inhibitor) plus paritaprevir/r (NS3/4A inhibitor codosed with ritonavir). Among 17 subtypes isolated from GT4-infected patients in the PEARL-I and AGATE-I studies, subtype prevalence by country of enrolment and country of origin suggested that subtypes 4a and 4d were likely circulating in Europe, while heterogeneous GT4 subtypes and a portion of GT4a detected in European and North American countries were likely due to immigration of HCV-infected patients from Africa. The distributions of birth cohort and race were also significantly different across GT4 subtypes 4a, 4d, and non-4a/4d. In addition, phylogenetic analyses of NS5A sequences revealed clustering within subtype 4a which segregated by the patient-reported country of origin and the presence of the L30R/S polymorphism. HCV NS5A sequences derived from GT4a-infected patients who originated from Europe and the United States clustered separately from sequences derived from patients who originated from Egypt, suggesting that genetically distinct strains of subtype 4a may be circulating globally. Finally, NS5A baseline polymorphisms were frequently detected at amino acid positions of interest for the inhibitor-class and OBV retained activity against 37 of 39 NS5A GT4 clinical isolates, with no impact on treatment outcome in the PEARL-I and AGATE-I studies.

Published
2018

4. Resistance characterization of hepatitis C virus genotype 2 from Japanese patients treated with ombitasvir and paritaprevir/ritonavir

Author

Katia Alves, Rebecca Redman, Tatyana Dekhtyar, Margaret Burroughs, Gretja Schnell, Lino Rodrigues-Jr, Rakesh Tripathi, Thomas Reisch, Michelle Irvin, Kazuaki Chayama, Tami Pilot-Matias, Preethi Krishnan, Christine Collins, Jill Beyer, Hiromitsu Kumada, and Carolyn M. Setze

Subjects
hepatitis C virus, Cyclopropanes, Male, 0301 basic medicine, viruses, Hepacivirus, Drug resistance, chemistry.chemical_compound, 0302 clinical medicine, Japan, Anilides, Treatment Failure, Research Articles, Sulfonamides, education.field_of_study, virus diseases, Valine, Hepatitis C, Middle Aged, Treatment Outcome, Infectious Diseases, Drug Therapy, Combination, Female, 030211 gastroenterology & hepatology, Research Article, medicine.drug, Macrocyclic Compounds, Genotype, Proline, Lactams, Macrocyclic, 030106 microbiology, Population, Antiviral Agents, 03 medical and health sciences, Virology, Drug Resistance, Viral, Ribavirin, medicine, genotype 2, Humans, education, Hepatitis, Polymorphism, Genetic, Ritonavir, business.industry, paritaprevir, Hepatitis C, Chronic, biochemical phenomena, metabolism, and nutrition, medicine.disease, digestive system diseases, Ombitasvir, ombitasvir, chemistry, Paritaprevir, Carbamates, business
Abstract

Treatment of HCV genotype (GT) 2-infected Japanese patients with paritaprevir (NS3/4A inhibitor boosted with ritonavir) and ombitasvir (NS5A inhibitor) without ribavirin for 12 weeks in the phase 2 study M12-536, and with ribavirin for 16 weeks in phase 3 study GIFT II resulted in SVR rates of 72.2% to 91.5%. Overall, 11 out of 125 patients with GT2a and 37 out of 79 patients with GT2b infection experienced virologic failure. The prevalence of baseline polymorphisms in NS3 and NS5A and their the impact on treatment outcome, as well as the development of viral resistance in GT2-infected patients experiencing virologic failure were evaluated by HCV NS3 and NS5A population and clonal sequence analyses. Baseline polymorphisms in NS3 that confer resistance to paritaprevir were rare in both GT2a- and GT2b-infected patients, while baseline polymorphisms in NS5A that confer resistance to ombitasvir were detected in 11.2% and 14.1% of the GT2a- and GT2b-infected patients, respectively. There was no significant impact of baseline polymorphisms on treatment outcome in Japanese patients. The most common treatment-emergent substitutions at the time of virologic failure occurred at amino acid positions 168 in NS3 and 28 in NS5A in both GT2a- and GT2b-infected patients. Although there was a higher rate of virologic failure in patients with GT2b infection, the resistance analyses presented in this report support the conclusion that testing for baseline resistance-associated polymorphisms is not warranted for HCV GT2-infected patients treated with a regimen of ombitasvir/paritaprevir/ritonavir + ribavirin for 16 weeks.

Published
2017

5. Synthesis and evaluation of 2'-dihalo ribonucleotide prodrugs with activity against hepatitis C virus

Author

Preethi Krishnan, Rodger F. Henry, Christopher C. Marvin, Tatyana Dekhtyar, Rolf Wagner, John T. Randolph, A. Chris Krueger, David A. Degoey, Vincent Peterkin, Michelle Irvin, Geoff T. Halvorsen, Jason P. Shanley, Heyman Howard R, Eric A. Voight, Robert A. Carr, Cecilia Van Handel, Tongmei Li, Brian S. Brown, Daniel A.J. Bow, Hui-Ju Chen, and DeAnne Stolarik

Subjects
Sofosbuvir, Hepatitis C virus, Clinical Biochemistry, Pharmaceutical Science, Hepacivirus, Microbial Sensitivity Tests, Pharmacology, medicine.disease_cause, Virus Replication, 01 natural sciences, Biochemistry, Antiviral Agents, chemistry.chemical_compound, Structure-Activity Relationship, In vivo, Drug Discovery, medicine, Humans, Prodrugs, Molecular Biology, NS5B, Uridine, Dose-Response Relationship, Drug, Molecular Structure, 010405 organic chemistry, Chemistry, Organic Chemistry, Phosphoramidate, Hepatitis C, Prodrug, medicine.disease, 0104 chemical sciences, 010404 medicinal & biomolecular chemistry, Hepatocytes, Molecular Medicine, Nucleoside, medicine.drug
Abstract

Download : Download high-res image (149KB) Download : Download full-size image Hepatitis C virus (HCV) nucleoside inhibitors have been a key focus of nearly 2 decades of HCV drug research due to a high barrier to drug resistance and pan-genotypic activity profile provided by molecules in this drug class. Our investigations focused on several potent 2′-halogenated uridine-based HCV polymerase inhibitors, resulting in the discovery of novel 2′-deoxy-2′-dihalo-uridine analogs that are potent inhibitors in replicon assays for all genotypes. Further studies to improve in vivo performance of these nucleoside inhibitors identified aminoisobutyric acid ethyl ester (AIBEE) phosphoramidate prodrugs 18a and 18c, which provide high levels of the active triphosphate in dog liver. AIBEE prodrug 18c was compared with sofosbuvir (1) by co-dosing both compounds by oral administration in dog (5 mg/kg each) and measuring liver concentrations of the active triphosphate metabolite at both 4 and 24 h post dosing. In this study, 18c provided liver triphosphate concentrations that were 6-fold higher than sofosbuvir (1) at both biopsy time points, suggesting that 18c could be a highly effective agent for treating HCV infected patients in the clinic.

Published
2019

6. Discovery of fluorobenzimidazole HCV NS5A inhibitors

Author

Nelson Lissa T, Tatyana Dekhtyar, DeAnne Stolarik, Thomas Reisch, Warren M. Kati, Donner Pamela L, Tami Pilot-Matias, Sachin V. Patel, Rolf Wagner, Preethi Krishnan, Douglas K. Hutchinson, Todd W. Rockway, Neeta Mistry, David W A Beno, Rubina Mondal, Clarence J. Maring, John T. Randolph, and Charles A. Flentge

Subjects
0301 basic medicine, Benzimidazole, Genotype, Halogenation, viruses, Hepacivirus, 030106 microbiology, Clinical Biochemistry, HCV genotypes, Pharmaceutical Science, Viral Nonstructural Proteins, Antiviral Agents, 01 natural sciences, Biochemistry, Mice, 03 medical and health sciences, chemistry.chemical_compound, Dogs, Drug Discovery, Animals, Humans, HCV NS5A Inhibitor, Replicon, NS5A, Molecular Biology, biology, 010405 organic chemistry, Organic Chemistry, virus diseases, biochemical phenomena, metabolism, and nutrition, biology.organism_classification, Hepatitis C, Virology, digestive system diseases, In vitro, Orders of magnitude (mass), Rats, 0104 chemical sciences, chemistry, Molecular Medicine, Benzimidazoles
Abstract

Research toward a next-generation HCV NS5A inhibitor has identified fluorobenzimidazole analogs that demonstrate potent, broad-genotype in vitro activity against HCV genotypes 1-6 replicons as well as HCV NS5A variants that are orders of magnitude less susceptible to inhibition by first-generation NS5A inhibitors in comparison to wild-type replicons. The fluorobenzimidazole inhibitors have improved pharmacokinetic properties in comparison to non-fluorinated benzimidazole analogs. Discovery of these inhibitors was facilitated by exploring SAR in a structurally simplified inhibitor series.

Published
2016

7. Discovery of 2-aminoisobutyric acid ethyl ester (AIBEE) phosphoramidate prodrugs for delivering nucleoside HCV NS5B polymerase inhibitors

Author

John T. Randolph, Vincent Peterkin, Robert A. Carr, David A. Degoey, Tongmei Li, Daniel A.J. Bow, Hui-Ju Chen, Preethi Krishnan, DeAnne Stolarik, Rolf Wagner, Cecilia Van Handel, Michelle Irvin, A. Chris Krueger, Heyman Howard R, and Tatyana Dekhtyar

Subjects
Aminoisobutyric Acids, Clinical Biochemistry, Pharmaceutical Science, Hepacivirus, Microbial Sensitivity Tests, Viral Nonstructural Proteins, Pharmacology, Virus Replication, Antiviral Agents, 01 natural sciences, Biochemistry, chemistry.chemical_compound, Dogs, Organophosphorus Compounds, Drug Discovery, medicine, Animals, Humans, Prodrugs, Enzyme Inhibitors, Molecular Biology, Polymerase, biology, medicine.diagnostic_test, 010405 organic chemistry, Chemistry, Organic Chemistry, Phosphoramidate, Metabolism, Prodrug, RNA-Dependent RNA Polymerase, Deoxyuridine, Uridine, In vitro, 0104 chemical sciences, 010404 medicinal & biomolecular chemistry, Liver, Liver biopsy, Hepatocytes, biology.protein, Molecular Medicine, Nucleoside
Abstract

Our HCV research program investigated novel 2′-dihalogenated nucleoside HCV polymerase inhibitors and identified compound 1, a 5′-phosphoramidate prodrug of 2′-deoxy-2′-α-bromo-β-chloro uridine. Although 1 had a favorable in vitro activity profile in HCV replicons, oral dosing in dog resulted in low levels of the active 5′-triphosphate (TP) in liver. Metabolism studies using human hepatocytes provided a simple assay for screening alternative phosphoramidate prodrug analogs. Compounds that produced high TP concentrations in hepatocytes were tested in dog liver biopsy studies. This method identified 2-aminoisobutyric acid ethyl ester (AIBEE) phosphoramidate prodrug 14, which provided 100-fold higher TP concentrations in dog liver in comparison to 1 (4 and 24 h after 5 mg/kg oral dose).

Published
2020

8. Resistance Analysis of a 3-Day Monotherapy Study with Glecaprevir or Pibrentasvir in Patients with Chronic Hepatitis C Virus Genotype 1 Infection

Author

Preethi Krishnan, Rakesh Tripathi, Liangjun Lu, Betty B. Yao, Tami Pilot-Matias, Armen Asatryan, Christine Collins, Federico J. Mensa, Jill Beyer, Michelle Irvin, Thomas Reisch, Jens Kort, Gretja Schnell, Eric Lawitz, Teresa I. Ng, Sandra S. Lovell, Tatyana Dekhtyar, and Campbell Andrew L

Subjects
0301 basic medicine, Cyclopropanes, Aminoisobutyric Acids, Pyrrolidines, viruses, lcsh:QR1-502, Hepacivirus, medicine.disease_cause, lcsh:Microbiology, 0302 clinical medicine, Genotype, Sulfonamides, virus diseases, glecaprevir, Viral Load, Pibrentasvir, Infectious Diseases, Liver, monotherapy, HCV, RNA, Viral, 030211 gastroenterology & hepatology, Drug Therapy, Combination, Proline, Hepatitis C virus, Lactams, Macrocyclic, 030106 microbiology, pibrentasvir, Antiviral Agents, Virus, Article, resistance, 03 medical and health sciences, Drug Resistance, Multiple, Viral, Leucine, Virology, Quinoxalines, medicine, Humans, Protease inhibitor (pharmacology), NS5A, NS3, business.industry, Glecaprevir, biochemical phenomena, metabolism, and nutrition, Hepatitis C, Chronic, Fibrosis, digestive system diseases, ABT-493, Amino Acid Substitution, ABT-530, Benzimidazoles, business
Abstract

Glecaprevir (an NS3/4A protease inhibitor) and pibrentasvir (an NS5A inhibitor) are potent and pangenotypic hepatitis C virus (HCV) direct-acting antivirals. This report describes the baseline polymorphisms and treatment-emergent substitutions in NS3 or NS5A detected in samples from HCV genotype 1-infected patients receiving 3-day monotherapy of glecaprevir or pibrentasvir, respectively. None of the NS3 polymorphisms detected in the 47 baseline samples collected prior to glecaprevir monotherapy conferred reduced susceptibility to glecaprevir. The NS3 A156T substitution, which conferred resistance to glecaprevir but had low replication efficiency, emerged in one genotype 1a-infected patient among the 35 patients with available post-baseline sequence data. Baseline NS5A polymorphisms were detected in 12 of 40 patients prior to pibrentasvir monotherapy, most polymorphisms were single-position NS5A amino acid substitutions that did not confer resistance to pibrentasvir. Among the 19 patients with available post-baseline NS5A sequence data, 3 had treatment-emergent NS5A substitutions during pibrentasvir monotherapy. All treatment-emergent NS5A substitutions were linked multiple-position, almost exclusively double-position, substitutions that conferred resistance to pibrentasvir. Replicons engineered with these double-position substitutions had low replication efficiency. In conclusion, resistance-conferring substitutions emerged in a small number of genotype 1-infected patients during glecaprevir or pibrentasvir monotherapy, unlike other NS5A inhibitors, pibrentasvir did not select single-position NS5A substitutions during monotherapy.

Published
2018

9. Pooled Resistance Analysis in Patients with Hepatitis C Virus Genotype 1 to 6 Infection Treated with Glecaprevir-Pibrentasvir in Phase 2 and 3 Clinical Trials

Author

Federico J. Mensa, Wangang Xie, Jill Beyer, Preethi Krishnan, Michelle Irvin, Rakesh Tripathi, Teresa I. Ng, Gretja Schnell, Lois Larsen, Tatyana Dekhtyar, Tami Pilot-Matias, Christine Collins, and Thomas Reisch

Subjects
0301 basic medicine, Cyclopropanes, medicine.medical_specialty, Cirrhosis, Aminoisobutyric Acids, Pyrrolidines, Sofosbuvir, Genotype, Proline, Sustained Virologic Response, viruses, Hepatitis C virus, Lactams, Macrocyclic, medicine.disease_cause, Gastroenterology, Antiviral Agents, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Leucine, Internal medicine, Quinoxalines, Drug Resistance, Viral, medicine, Humans, Pharmacology (medical), NS5A, Pharmacology, Sulfonamides, Polymorphism, Genetic, business.industry, Ribavirin, Glecaprevir, Hepatitis C, Chronic, medicine.disease, Pibrentasvir, Regimen, 030104 developmental biology, Infectious Diseases, chemistry, 030211 gastroenterology & hepatology, Benzimidazoles, business, medicine.drug
Abstract

Over 2,200 patients infected with hepatitis C virus (HCV) genotypes (GT) 1 to 6, with or without cirrhosis, who were treatment naive or experienced to interferon, ribavirin, and/or sofosbuvir were treated with glecaprevir/pibrentasvir for 8, 12, or 16 weeks in eight registrational phase 2 and 3 clinical studies. High rates of sustained virologic response at 12 weeks postdosing (SVR12) were achieved with a

Published
2018

10. Highlights of the Structure-Activity Relationships of Benzimidazole Linked Pyrrolidines Leading to the Discovery of the Hepatitis C Virus NS5A Inhibitor Pibrentasvir (ABT-530)

Author

Ryan G. Keddy, Warren M. Kati, Tami Pilot-Matias, Nelson Lissa T, DeAnne Stolarik, Tatyana Dekhtyar, Rubina Mondal, Thomas Reisch, A. Chris Krueger, Hutchinson Douglas K, Donner Pamela L, John T. Randolph, Wenqing Gao, David A. Betebenner, Clarence J. Maring, Preethi Krishnan, Neeta S. Panchal, Christine A. Collins, Todd W. Rockway, Yi Gao, Teresa I. Ng, David W A Beno, John K. Pratt, Dachun Liu, Sachin V. Patel, Charles A. Flentge, Mark A. Matulenko, and Rolf Wagner

Subjects
Pyrrolidines, Genotype, viruses, Hepatitis C virus, Hepacivirus, medicine.disease_cause, Virus Replication, Antiviral Agents, Virus, 03 medical and health sciences, chemistry.chemical_compound, Mice, Structure-Activity Relationship, 0302 clinical medicine, Interferon, Drug Discovery, medicine, Animals, Tissue Distribution, NS5A, biology, Chemistry, Ribavirin, virus diseases, biochemical phenomena, metabolism, and nutrition, biology.organism_classification, Virology, digestive system diseases, Ombitasvir, Pibrentasvir, 030220 oncology & carcinogenesis, Drug Design, Molecular Medicine, 030211 gastroenterology & hepatology, Benzimidazoles, medicine.drug
Abstract

Curative interferon and ribavirin sparing treatments for hepatitis C virus (HCV)-infected patients require a combination of mechanistically orthogonal direct acting antivirals. A shared component of these treatments is usually an HCV NS5A inhibitor. First generation FDA approved treatments, including the component NS5A inhibitors, do not exhibit equivalent efficacy against HCV virus genotypes 1-6. In particular, these first generation NS5A inhibitors tend to select for viral drug resistance. Ombitasvir is a first generation HCV NS5A inhibitor included as a key component of Viekira Pak for the treatment of patients with HCV genotype 1 infection. Since the launch of next generation HCV treatments, functional cure for genotype 1-6 HCV infections has been achieved, as well as shortened treatment duration across a wider spectrum of genotypes. In this paper, we show how we have modified the anchor, linker, and end-cap architecture of our NS5A inhibitor design template to discover a next generation NS5A inhibitor pibrentasvir (ABT-530), which exhibits potent inhibition of the replication of wild-type genotype 1-6 HCV replicons, as well as improved activity against replicon variants demonstrating resistance against first generation NS5A inhibitors.

Published
2018

11. In Vitro Antiviral Activity and Resistance Profile of the Next-Generation Hepatitis C Virus NS3/4A Protease Inhibitor Glecaprevir

Author

Preethi Krishnan, Rakesh Tripathi, Gretja Schnell, Jun Ma, Timothy Middleton, Todd Hopkins, Ron Pithawalla, Tami Pilot-Matias, Tatyana Dekhtyar, Li-Juan Jiang, Thomas Reisch, Michelle Irvin, Yat Sun Or, Christine Collins, Guoqiang Wang, Keith F. McDaniel, Dale J. Kempf, Jill Beyer, Teresa I. Ng, and Liangjun Lu

Subjects
0301 basic medicine, Proteases, medicine.medical_treatment, Hepatitis C virus, viruses, medicine.disease_cause, Antiviral Agents, resistance, 03 medical and health sciences, 0302 clinical medicine, medicine, Pharmacology (medical), Protease inhibitor (pharmacology), Pharmacology, NS3, Protease, Chemistry, virus diseases, Glecaprevir, glecaprevir, biochemical phenomena, metabolism, and nutrition, Virology, Pibrentasvir, digestive system diseases, NS2-3 protease, ABT-493, 030104 developmental biology, Infectious Diseases, NS3/4A protease inhibitor, HCV, antiviral activity, 030211 gastroenterology & hepatology
Abstract

Glecaprevir (formerly ABT-493) is a novel hepatitis C virus (HCV) NS3/4A protease inhibitor (PI) with pangenotypic activity. It inhibited the enzymatic activity of purified NS3/4A proteases from HCV genotypes 1 to 6 in vitro (half-maximal [50%] inhibitory concentration = 3.5 to 11.3 nM) and the replication of stable HCV subgenomic replicons containing proteases from genotypes 1 to 6 (50% effective concentration [EC 50 ] = 0.21 to 4.6 nM). Glecaprevir had a median EC 50 of 0.30 nM (range, 0.05 to 3.8 nM) for HCV replicons containing proteases from 40 samples from patients infected with HCV genotypes 1 to 5. Importantly, glecaprevir was active against the protease from genotype 3, the most-difficult-to-treat HCV genotype, in both enzymatic and replicon assays demonstrating comparable activity against the other HCV genotypes. In drug-resistant colony selection studies, glecaprevir generally selected substitutions at NS3 amino acid position A156 in replicons containing proteases from genotypes 1a, 1b, 2a, 2b, 3a, and 4a and substitutions at position D/Q168 in replicons containing proteases from genotypes 3a, 5a, and 6a. Although the substitutions A156T and A156V in NS3 of genotype 1 reduced susceptibility to glecaprevir, replicons with these substitutions demonstrated a low replication efficiency in vitro . Glecaprevir is active against HCV with most of the common NS3 amino acid substitutions that are associated with reduced susceptibility to other currently approved HCV PIs, including those at positions 155 and 168. Combination of glecaprevir with HCV inhibitors with other mechanisms of action resulted in additive or synergistic antiviral activity. In summary, glecaprevir is a next-generation HCV PI with potent pangenotypic activity and a high barrier to the development of resistance.

Published
2017

12. Hepatitis C Virus Genotype 4 Resistance and Subtype Demographic Characterization of Patients Treated with Ombitasvir plus Paritaprevir/Ritonavir

Author

Coleen Hall, Liangjun Lu, Tami Pilot-Matias, Thomas Reisch, Christine Collins, Rakesh Tripathi, Tatyana Dekhtyar, Regis A. Vilchez, Preethi Krishnan, Gretja Schnell, and Jill Beyer

Subjects
Adult, Cyclopropanes, Male, Macrocyclic Compounds, Genotype, Proline, Hepacivirus, Hepatitis C virus, viruses, Lactams, Macrocyclic, medicine.disease_cause, Antiviral Agents, chemistry.chemical_compound, Young Adult, Drug Resistance, Viral, medicine, Humans, Pharmacology (medical), Anilides, NS5A, Phylogeny, Pharmacology, Sulfonamides, Ritonavir, biology, Ribavirin, virus diseases, Valine, Hepatitis C, biochemical phenomena, metabolism, and nutrition, Hepatitis C, Chronic, Middle Aged, medicine.disease, biology.organism_classification, Virology, Ombitasvir, digestive system diseases, Infectious Diseases, Treatment Outcome, chemistry, Paritaprevir, Drug Therapy, Combination, Female, Carbamates, medicine.drug
Abstract

Hepatitis C virus (HCV) genotype 4 (GT4) is genetically diverse, with 17 confirmed subtypes, and comprises approximately 13% of infections worldwide. In this study, we identified GT4 subtypes by phylogenetic analysis, assessed differences in patient demographics across GT4 subtypes, examined baseline sequence variability among subtypes and the potential impact on treatment outcome, and analyzed the development of viral resistance in patients who received a regimen of ombitasvir (nonstructural protein 5A [NS5A] inhibitor) plus ritonavir-boosted paritaprevir (NS3/4A inhibitor) with or without ribavirin (RBV) for the treatment of HCV GT4 infection. Phylogenetic analysis of HCV NS3/4A, NS5A, and NS5B nucleotide sequences identified 7 subtypes (4a, 4b, 4c, 4d, 4f, 4g/4k, and 4o) among 132 patient samples. Subtype prevalence varied by country, and the distributions of patient birth cohort and race were significantly different across GT4 subtypes 4a, 4d, and non-4a/4d. Baseline amino acid variability was detected in NS5A across GT4 subtypes but had no impact on treatment outcome. Three patients experienced virologic failure and were infected with subtype 4d, and the predominant resistance-associated variants at the time of failure were D168V in NS3 and L28V in NS5A. Overall, high response rates were observed among patients infected with 7 HCV GT4 subtypes, with no impact of baseline variants on treatment outcome. GT4 subtype distribution in this study differed based on patient demographics and geography.

Published
2015

13. In Vitro and In Vivo Antiviral Activity and Resistance Profile of the Hepatitis C Virus NS3/4A Protease Inhibitor ABT-450

Author

Rakesh Tripathi, Liangjun Lu, Tatyana Dekhtyar, Tami Pilot-Matias, Todd Hopkins, Teresa Ng, Christine Collins, Rajeev M. Menon, Thomas Reisch, Michelle Irvin, Dale J. Kempf, Timothy Middleton, Yat Sun Or, Ron Pithawalla, Keith F. McDaniel, Isabelle A. Gaultier, Akhteruzzaman Molla, and Daniel E. Cohen

Subjects
Cyclopropanes, Macrocyclic Compounds, Proline, Lactams, Macrocyclic, Hepatitis C virus, medicine.medical_treatment, Hepacivirus, Drug resistance, Viral Nonstructural Proteins, Pharmacology, Biology, medicine.disease_cause, Antiviral Agents, Ombitasvir/paritaprevir/ritonavir, Drug Resistance, Viral, Genotype, medicine, Humans, Pharmacology (medical), Sulfonamides, NS3, Protease, Hepatitis C, medicine.disease, Virology, Infectious Diseases, Ritonavir, medicine.drug
Abstract

The development of direct-acting antiviral agents is a promising therapeutic advance in the treatment of hepatitis C virus (HCV) infection. However, rapid emergence of drug resistance can limit efficacy and lead to cross-resistance among members of the same drug class. ABT-450 is an efficacious inhibitor of HCV NS3/4A protease, with 50% effective concentration values of 1.0, 0.21, 5.3, 19, 0.09, and 0.69 nM against stable HCV replicons with NS3 protease from genotypes 1a, 1b, 2a, 3a, 4a, and 6a, respectively. In vitro , the most common amino acid variants selected by ABT-450 in genotype 1 were located in NS3 at positions 155, 156, and 168, with the D168Y variant conferring the highest level of resistance to ABT-450 in both genotype 1a and 1b replicons (219- and 337-fold, respectively). In a 3-day monotherapy study with HCV genotype 1-infected patients, ABT-450 was coadministered with ritonavir, a cytochrome P450 3A4 inhibitor shown previously to markedly increase peak, trough, and overall drug exposures of ABT-450. A mean maximum HCV RNA decline of 4.02 log 10 was observed at the end of the 3-day dosing period across all doses. The most common variants selected in these patients were R155K and D168V in genotype 1a and D168V in genotype 1b. However, selection of resistant variants was significantly reduced at the highest ABT-450 dose compared to lower doses. These findings were informative for the subsequent evaluation of ABT-450 in combination with additional drug classes in clinical trials in HCV-infected patients. (Study M11-602 is registered at ClinicalTrials.gov under registration no. NCT01074008.)

Published
2015

14. Integrated Resistance Analysis of CERTAIN-1 and CERTAIN-2 Studies in Hepatitis C Virus-Infected Patients Receiving Glecaprevir and Pibrentasvir in Japan

Author

Margaret Burroughs, Kazuaki Chayama, Wangang Xie, Bo Fu, Preethi Krishnan, Thomas Reisch, Tami Pilot-Matias, Tatyana Dekhtyar, Hiromitsu Kumada, Christine Collins, Rebecca Redman, Michelle Irvin, Rakesh Tripathi, Gretja Schnell, and Jill Beyer

Subjects
0301 basic medicine, Cyclopropanes, Liver Cirrhosis, Male, Aminoisobutyric Acids, Pyrrolidines, viruses, Drug resistance, Hepacivirus, Viral Nonstructural Proteins, medicine.disease_cause, Gastroenterology, 0302 clinical medicine, Japan, Pharmacology (medical), Sulfonamides, NS5A inhibitor, virus diseases, Hepatitis C, glecaprevir, Pibrentasvir, Infectious Diseases, HCV, 030211 gastroenterology & hepatology, Drug Therapy, Combination, Female, Viral hepatitis, medicine.drug, medicine.medical_specialty, Daclatasvir, Genotype, Proline, Hepatitis C virus, Lactams, Macrocyclic, 030106 microbiology, pibrentasvir, protease inhibitors, Antiviral Agents, 03 medical and health sciences, Leucine, Internal medicine, Quinoxalines, Drug Resistance, Viral, medicine, Humans, Pharmacology, business.industry, Glecaprevir, biochemical phenomena, metabolism, and nutrition, Hepatitis C, Chronic, medicine.disease, Isoquinolines, digestive system diseases, Regimen, Benzimidazoles, business
Abstract

Glecaprevir and pibrentasvir are hepatitis C virus (HCV) pangenotypic inhibitors targeting NS3/4A protease and NS5A, respectively. This once-daily, fixed-dose combination regimen demonstrated high sustained virologic response 12 weeks postdosing (SVR 12 ) rates in CERTAIN-1 and CERTAIN-2 studies in Japanese HCV-infected patients, with a low virologic failure rate (1.2%). There were no virologic failures among direct-acting antiviral (DAA)-treatment-naive genotype 1a (GT1a) ( n = 4)-, GT1b ( n = 128)-, and GT2 ( n = 97)-infected noncirrhotic patients treated for 8 weeks or among GT1b ( n = 38)- or GT2 ( n = 20)-infected patients with compensated cirrhosis treated for 12 weeks. Two of 33 DAA-experienced and 2 of 12 GT3-infected patients treated for 12 weeks experienced virologic failure. Pooled resistance analysis, grouped by HCV subtype, treatment duration, prior treatment experience, and cirrhosis status, was conducted. Among DAA-naive GT1b-infected patients, the baseline prevalence of NS3-D168E was 1.2%, that of NS5A-L31M was 3.6%, and that of NS5A-Y93H was 17.6%. Baseline polymorphisms in NS3 or NS5A were less prevalent in GT2, with the exception of the common L/M31 polymorphism in NS5A. Among DAA-experienced GT1b-infected patients (30/32 daclatasvir plus asunaprevir-experienced patients), the baseline prevalence of NS3-D168E/T/V was 48.4%, that of NS5A-L31F/I/M/V was 81.3%, that of the NS5A P32deletion was 6.3%, and that of NS5A-Y93H was 59.4%. Common baseline polymorphisms in NS3 and/or NS5A had no impact on treatment outcomes in GT1- and GT2-infected patients; the impact on GT3-infected patients could not be assessed due to the enrollment of patients infected with diverse subtypes and the limited number of patients. The glecaprevir-pibrentasvir combination regimen allows a simplified treatment option without the need for HCV subtyping or baseline resistance testing for DAA-naive GT1- or GT2-infected patients. (The CERTAIN-1 and CERTAIN-2 studies have been registered at ClinicalTrials.gov under identifiers NCT02707952 and NCT02723084, respectively.)

Published
2017

15. In Vitro Antiviral Activity and Resistance Profile of the Next-Generation Hepatitis C Virus NS5A Inhibitor Pibrentasvir

Author

Tami Pilot-Matias, Preethi Krishnan, Jill Beyer, Christine Collins, Thomas Reisch, John T. Randolph, Rolf Wagner, Rakesh Tripathi, Gretja Schnell, Tatyana Dekhtyar, Michelle Irvin, Warren M. Kati, Clarence J. Maring, Liangjun Lu, and Teresa I. Ng

Subjects
0301 basic medicine, viruses, Hepatitis C virus, pibrentasvir, 030106 microbiology, Drug resistance, Biology, medicine.disease_cause, Antiviral Agents, resistance, 03 medical and health sciences, 0302 clinical medicine, Genotype, medicine, Pharmacology (medical), Replicon, NS5A, Pharmacology, chemistry.chemical_classification, NS5A inhibitor, virus diseases, Glecaprevir, biochemical phenomena, metabolism, and nutrition, Virology, digestive system diseases, Pibrentasvir, Amino acid, Infectious Diseases, chemistry, ABT-530, HCV, antiviral activity, 030211 gastroenterology & hepatology
Abstract

Pibrentasvir (ABT-530) is a novel and pan-genotypic hepatitis C virus (HCV) NS5A inhibitor with 50% effective concentration (EC 50 ) values ranging from 1.4 to 5.0 pM against HCV replicons containing NS5A from genotypes 1 to 6. Pibrentasvir demonstrated similar activity against a panel of chimeric replicons containing HCV NS5A of genotypes 1 to 6 from clinical samples. Resistance selection studies were conducted using HCV replicon cells with NS5A from genotype 1a, 1b, 2a, 2b, 3a, 4a, 5a, or 6a at a concentration of pibrentasvir that was 10- or 100-fold over its EC 50 for the respective replicon. With pibrentasvir at 10-fold over the respective EC 50 , only a small number of colonies (0.00015 to 0.0065% of input cells) with resistance-associated amino acid substitutions were selected in replicons containing genotype 1a, 2a, or 3a NS5A, and no viable colonies were selected in replicons containing NS5A from other genotypes. With pibrentasvir at 100-fold over the respective EC 50 , very few colonies (0.0002% of input cells) were selected by pibrentasvir in genotype 1a replicon cells while no colonies were selected in other replicons. Pibrentasvir is active against common resistance-conferring substitutions in HCV genotypes 1 to 6 that were identified for other NS5A inhibitors, including those at key amino acid positions 28, 30, 31, or 93. The combination of pibrentasvir with HCV inhibitors of other classes produced synergistic inhibition of HCV replication. In summary, pibrentasvir is a next-generation HCV NS5A inhibitor with potent and pan-genotypic activity, and it maintains activity against common amino acid substitutions of HCV genotypes 1 to 6 that are known to confer resistance to currently approved NS5A inhibitors.

Published
2017

16. Resistance analysis in the MAGELLAN-1 Study (Part 2): glecaprevir/pibrentasvir therapy in HCV-infected patients who had failed prior DAA regimens containing NS3/4A protease and/or NS5A inhibitors

Author

Armen Asatryan, Thomas Reisch, Rakesh Tripathi, Gretja Schnell, Preethi Krishnan, Tatyana Dekhtyar, Y. Lei, Tami Pilot-Matias, Teresa I. Ng, Michelle Irvin, Federico J. Mensa, Christine Collins, and Jill Beyer

Subjects
0301 basic medicine, 03 medical and health sciences, 030104 developmental biology, 0302 clinical medicine, Hepatology, business.industry, Medicine, 030211 gastroenterology & hepatology, Glecaprevir / pibrentasvir, NS5A, business, Virology, Ns3 4a protease
Published
2017

17. P1-Substituted Symmetry-Based Human Immunodeficiency Virus Protease Inhibitors with Potent Antiviral Activity against Drug-Resistant Viruses

Author

Akhteruzzaman Molla, David A. Degoey, Dale J. Kempf, William J. Flosi, Vincent S. Stoll, Tatyana Dekhtyar, David J. Grampovnik, Larry L. Klein, Hui Ju Chen, and Mulugeta Mamo

Subjects
Models, Molecular, medicine.medical_treatment, Biological Availability, Drug resistance, In Vitro Techniques, Pharmacology, Crystallography, X-Ray, Virus, Structure-Activity Relationship, Pharmacotherapy, Pharmacokinetics, Drug Resistance, Viral, Drug Discovery, medicine, Animals, HIV Protease Inhibitor, Structure–activity relationship, Potency, Protease, Chemistry, virus diseases, Hydrogen Bonding, Stereoisomerism, HIV Protease Inhibitors, Virology, Rats, Mutation, HIV-1, Microsomes, Liver, Molecular Medicine
Abstract

Because there is currently no cure for HIV infection, patients must remain on long-term drug therapy, leading to concerns over potential drug side effects and the emergence of drug resistance. For this reason, new and safe antiretroviral agents with improved potency against drug-resistant strains of HIV are needed. A series of HIV protease inhibitors (PIs) with potent activity against both wild-type (WT) virus and drug-resistant strains of HIV was designed and synthesized. The incorporation of substituents with hydrogen bond donor and acceptor groups at the P1 position of our symmetry-based inhibitor series resulted in significant potency improvements against the resistant mutants. By this approach, several compounds, such as 13, 24, and 29, were identified that demonstrated similar or improved potencies compared to 1 against highly mutated strains of HIV derived from patients who previously failed HIV PI therapy. Overall, compound 13 demonstrated the best balance of potency against drug resistant strains of HIV and oral bioavailability in pharmacokinetic studies. X-ray analysis of an HIV PI with an improved resistance profile bound to WT HIV protease is also reported.

Published
2011

18. Hepatitis C virus genetic diversity by geographic region within genotype 1-6 subtypes among patients treated with glecaprevir and pibrentasvir

Author

Tami Pilot-Matias, Tatyana Dekhtyar, Christine Collins, Michelle Irvin, Gretja Schnell, Thomas Reisch, Rakesh Tripathi, Jill Beyer, Liangjun Lu, Wangang Xie, Teresa I. Ng, and Preethi Krishnan

Subjects
Cyclopropanes, Aminoisobutyric Acids, Pyrrolidines, viruses, Population Dynamics, lcsh:Medicine, Hepacivirus, Viral Nonstructural Proteins, medicine.disease_cause, Geographical locations, Database and Informatics Methods, 0302 clinical medicine, Genotype, 030212 general & internal medicine, lcsh:Science, Phylogeny, Data Management, Genetics, Sulfonamides, Multidisciplinary, Geography, Phylogenetic tree, virus diseases, Phylogenetic Analysis, Pibrentasvir, Phylogenetics, Europe, Phylogeography, Biogeography, 030211 gastroenterology & hepatology, Sequence Analysis, Research Article, Computer and Information Sciences, Proline, Bioinformatics, Lactams, Macrocyclic, Hepatitis C virus, Biology, Research and Analysis Methods, 03 medical and health sciences, Leucine, Quinoxalines, Drug Resistance, Viral, Genetic variation, medicine, Humans, Evolutionary Systematics, Taxonomy, Evolutionary Biology, Genetic diversity, Population Biology, lcsh:R, Ecology and Environmental Sciences, Genetic Variation, Biology and Life Sciences, Glecaprevir, Hepatitis C, Chronic, biochemical phenomena, metabolism, and nutrition, Geographic Distribution, digestive system diseases, Regional Geography, Amino Acid Substitution, North America, Earth Sciences, lcsh:Q, Benzimidazoles, People and places, Population Genetics
Abstract

Hepatitis C virus (HCV) is genetically diverse and includes 7 genotypes and 67 confirmed subtypes, and the global distribution of each HCV genotype (GT) varies by geographic region. In this report, we utilized a large dataset of NS3/4A and NS5A sequences isolated from 2348 HCV GT1-6-infected patients treated with the regimen containing glecaprevir/pibrentasvir (GLE/PIB) to assess genetic diversity within HCV subtypes by geographic region using phylogenetic analyses, and evaluated the prevalence of baseline amino acid polymorphisms in NS3 and NS5A by region/country and phylogenetic cluster. Among 2348 NS3/4A and NS5A sequences, phylogenetic analysis identified 6 genotypes and 44 subtypes, including 3 GT1, 8 GT2, 3 GT3, 13 GT4, 1 GT5, and 16 GT6 subtypes. Phylogenetic analysis of HCV subtype 1a confirmed the presence of two clades, which differed by geographic region distribution and NS3 Q80K prevalence. We detected phylogenetic clustering by country in HCV subtypes 1a, 1b, 2a, 2b, and 5a, suggesting that genetically distinct virus lineages are circulating in different countries. In addition, two clades were detected in HCV GT4a and GT6e, and NS5A amino acid polymorphisms were differentially distributed between the 2 clades in each subtype. The prevalence of NS3 and NS5A baseline polymorphisms varied substantially by genotype and subtype; therefore, we also determined the activity of GLE or PIB against replicons containing NS3/4A or NS5A from HCV GT1-6 clinical samples representing 6 genotypes and 21 subtypes overall. GLE and PIB retained activity against the majority of HCV replicons containing NS3/4A or NS5A from HCV GT1-6 clinical samples, with a median EC50 of 0.29 nM for GLE and 1.1 pM for PIB in a transient replicon assay. The data presented in this report expands the available data on HCV epidemiology, subtype diversity by geographic region, and NS3 and NS5A baseline polymorphism prevalence.

Published
2018

19. Characterization of a Novel Human Immunodeficiency Virus Type 1 Protease Inhibitor, A-790742

Author

Dale J. Kempf, Liangjun Lu, David A. Degoey, William J. Flosi, Teresa I. Ng, Sherie Masse, Tatyana Dekhtyar, David J. Grampovnik, Larry L. Klein, and Akhteruzzaman Molla

Subjects
Proteases, medicine.medical_treatment, Microbial Sensitivity Tests, Pyrimidinones, Biology, Antiviral Agents, Lopinavir, HIV Protease, Drug Resistance, Viral, medicine, Humans, HIV Protease Inhibitor, Pharmacology (medical), Protease inhibitor (pharmacology), Selection, Genetic, Serial Passage, Pharmacology, Protease, Wild type, virus diseases, HIV Protease Inhibitors, Virology, NS2-3 protease, Phenotype, Infectious Diseases, Mutation, HIV-1, Ritonavir, medicine.drug
Abstract

A-790742 is a potent human immunodeficiency virus type 1 (HIV-1) protease inhibitor, with 50% effective concentrations ranging from 2 to 7 nM against wild-type HIV-1. The activity of this compound is lowered by approximately sevenfold in the presence of 50% human serum. A-790742 maintained potent antiviral activity against lopinavir-resistant variants generated in vitro as well as against a panel of molecular clones containing proteases derived from HIV-1 patient isolates with multiple protease mutations. During in vitro selection, A-790742 selected two primary mutations (V82L and I84V) along with L23I, L33F, K45I, A71V/A, and V77I in the pNL4-3 background and two other mutations (A71V and V82G) accompanied by M46I and L63P in the HIV-1 RF background. HIV-1 pNL4-3 clones with a single V82L or I84V mutation were phenotypically resistant to A-790742 and ritonavir. Taking these results together, A-790742 displays a favorable anti-HIV-1 profile against both the wild type and a large number of mutants resistant to other protease inhibitors. The selection of the uncommon V82L and V82G mutations in protease by A-790742 suggests the potential for an advantageous resistance profile with this protease inhibitor.

Published
2008

20. In Vitro Selection and Characterization of Human Immunodeficiency Virus Type 2 with Decreased Susceptibility to Lopinavir

Author

Dale J. Kempf, Tatyana Dekhtyar, Akhteruzzaman Molla, Hongmei Mo, Xiaozhi Lu, George J. Hanna, Gennadiy Koev, Barry Bernstein, Sherie Masse, Liangjun Lu, and Feng Gao

Subjects
Anti-HIV Agents, Molecular Sequence Data, Mutant, HIV Core Protein p24, Pyrimidinones, Biology, Virus Replication, Antiviral Agents, Lopinavir, Virus, Cell Line, Cytopathogenic Effect, Viral, Drug Resistance, Viral, medicine, Humans, HIV Protease Inhibitor, Pharmacology (medical), Protease inhibitor (pharmacology), Amino Acid Sequence, Pharmacology, virus diseases, RNA-Directed DNA Polymerase, HIV Protease Inhibitors, Virology, Atazanavir, Phenotype, Infectious Diseases, Viral replication, HIV-2, Mutagenesis, Site-Directed, Saquinavir, medicine.drug
Abstract

Lopinavir (LPV)-ritonavir has demonstrated durable antiviral activity in human immunodeficiency virus type 1 (HIV-1)-infected antiretroviral-naïve and protease inhibitor (PI)-experienced patients. However, information on LPV activity against HIV-2 and the patterns of mutations in HIV-2 in response to selection by LPV is limited. The activity of LPV against three strains of HIV-2 was assessed and compared to activity against a reference HIV-1 strain. LPV demonstrated activity similar to that observed against HIV-1 in two HIV-2 strains (HIV-2MSand HIV-2CBL-23) tested. On the other hand, approximately 10-fold-reduced susceptibility was observed with the third HIV-2 strain, HIV-2CDC310319. Passage of HIV-2MSwith increasing concentrations of LPV selected mutations V47A and D17N in the HIV-2 protease gene. The introduction of both 17N and 47A either individually or together into HIV-2RODmolecular infectious clones showed that the single V47A substitution in HIV-2 resulted in a substantial reduction in susceptibility to LPV. In contrast, this mutant retained wild-type susceptibility to other PIs and appeared to be hypersusceptible to atazanavir and saquinavir.

Published
2007

21. Discovery of imidazolidine-2,4-dione-linked HIV protease inhibitors with activity against lopinavir-resistant mutant HIV

Author

Hong Mei Mo, David J. Grampovnik, Larry L. Klein, David A. Degoey, Kennan C. Marsh, Tatyana Dekhtyar, Dale J. Kempf, Sherie Masse, Hui Ju Chen, and William J. Flosi

Subjects
Magnetic Resonance Spectroscopy, medicine.medical_treatment, Clinical Biochemistry, Pharmaceutical Science, HIV Infections, Pyrimidinones, Pharmacology, Crystallography, X-Ray, Imidazolidines, Biochemistry, Lopinavir, Structure-Activity Relationship, chemistry.chemical_compound, immune system diseases, Imidazolidine, Serial passage, Drug Resistance, Viral, Drug Discovery, medicine, Humans, HIV Protease Inhibitor, Protease inhibitor (pharmacology), Molecular Biology, Protease, biology, Chemistry, Organic Chemistry, virus diseases, HIV Protease Inhibitors, Virology, Enzyme inhibitor, Drug Design, Mutation, HIV-1, biology.protein, Molecular Medicine, Ritonavir, medicine.drug
Abstract

A new series of HIV protease inhibitors has been designed and synthesized based on the combination of the (R)-(hydroxyethylamino)sulfonamide isostere and the cyclic urea component of lopinavir. The series was optimized by replacing the 6-membered cyclic urea linker with an imidazolidine-2,4-dione which readily underwent N-alkylation to incorporate various methylene-linked heterocycle groups that bind favorably in site 3 of HIV protease. Significant improvements compared to lopinavir were seen in cell culture activity versus wild-type virus (pNL4-3) and the lopinavir-resistant mutant virus A17 (generated by in vitro serial passage of HIV-1 (pNL4-3) in MT-4 cells). Select imidazolidine-2,4-dione containing PIs were also more effective at inhibiting highly resistant patient isolates Pt1 and Pt2 than lopinavir. Pharmacokinetic data collected for compounds in this series varied considerably when coadministered orally in the rat with an equal amount of ritonavir (5 mg/kg each). The AUC values ranged from 0.144 to 12.33 microg h/mL.

Published
2006

22. Mutations Conferring Resistance to a Hepatitis C Virus (HCV) RNA-Dependent RNA Polymerase Inhibitor Alone or in Combination with an HCV Serine Protease Inhibitor In Vitro

Author

Vincent S. Stoll, Clarence J. Maring, Teresa Ng, Tatyana Dekhtyar, Todd W. Rockway, Sherie Masse, Pam Donner, Gennadiy Koev, Liangjun Lu, Akhteruzzaman Molla, Tami Pilot-Matias, Rubina Mondal, Kent D. Stewart, John K. Pratt, Hongmei Mo, and Ron Pithawalla

Subjects
Models, Molecular, Serine Proteinase Inhibitors, viruses, Hepatitis C virus, RNA-dependent RNA polymerase, Hepacivirus, Biology, medicine.disease_cause, Antiviral Agents, Cell Line, chemistry.chemical_compound, RNA polymerase, Drug Resistance, Viral, medicine, Pharmacology (medical), Protease inhibitor (pharmacology), Replicon, Enzyme Inhibitors, Pharmacology, NS3, Binding Sites, Molecular Structure, virus diseases, biochemical phenomena, metabolism, and nutrition, RNA-Dependent RNA Polymerase, Virology, Molecular biology, digestive system diseases, NS2-3 protease, Infectious Diseases, chemistry, RNA Polymerase Inhibitor, Mutation, RNA, Viral, Protein Binding
Abstract

Compounds A-782759 (an N -1-aza-4-hydroxyquinolone benzothiadiazine) and BILN-2061 are specific anti-hepatitis C virus (HCV) agents that inhibit the RNA-dependent RNA polymerase and the NS3 serine protease, respectively. Both compounds display potent activity against HCV replicons in tissue culture. In order to characterize the development of resistance to these anti-HCV agents, HCV subgenomic 1b-N replicon cells were cultured with A-782759 alone or in combination with BILN-2061 at concentrations 10 times above their corresponding 50% inhibitory concentrations in the presence of neomycin. Single substitutions in the NS5B polymerase gene (H95Q, N411S, M414L, M414T, or Y448H) resulted in substantial decreases in susceptibility to A-782759. Similarly, replicons containing mutations in the NS5B polymerase gene (M414L or M414T), together with single mutations in the NS3 protease gene (A156V or D168V), conferred high levels of resistance to both A-782759 and BILN-2061. However, the A-782759-resistant mutants remained susceptible to nucleoside and two other classes of nonnucleoside NS5B polymerase inhibitors, as well as interferon. In addition, we found that the frequency of replicons resistant to both compounds was significantly lower than the frequency of resistance to the single compound. Furthermore, the dually resistant mutants displayed significantly reduced replication capacities compared to the wild-type replicon. These findings provide strategic guidance for the future treatment of HCV infection.

Published
2005

23. Synthesis and antiviral activity of P1′ arylsulfonamide azacyclic urea HIV protease inhibitors

Author

Tatyana Dekhtyar, Larry L. Klein, Dale J. Kempf, Peggy P. Huang, Sudthida Vasavanonda, Vincent S. Stoll, and Randolph John T

Subjects
Models, Molecular, Stereochemistry, Clinical Biochemistry, Molecular Conformation, Pharmaceutical Science, Plasma protein binding, Biochemistry, Chemical synthesis, chemistry.chemical_compound, Structure-Activity Relationship, Drug Discovery, Hydrolase, Humans, Urea, HIV Protease Inhibitor, Protease inhibitor (pharmacology), Molecular Biology, chemistry.chemical_classification, Sulfonamides, biology, Organic Chemistry, Active site, Biological activity, General Medicine, HIV Protease Inhibitors, Sulfonamide, Enzyme, chemistry, biology.protein, Molecular Medicine
Abstract

A series of novel azacyclic urea HIV protease inhibitors bearing a benzenesulfonamide group at P1′ were synthesized utilizing a parallel synthesis method. Structural studies of early analogs bound in the enzyme active site were used to design more potent inhibitors. The effects of substituting the P1′ benzenesulfonyl group on antiviral activity and protein binding are described.

Published
2004

24. Analysis of HCV Genotype 2 and 3 Variants in Patients Treated with Combination Therapy of Next Generation HCV Direct-Acting Antiviral Agents ABT-493 and ABT-530

Author

Stanley Wang, Rakesh Tripathi, Tami Pilot-Matias, Thomas Reisch, Federico J. Mensa, Teresa I. Ng, Tatyana Dekhtyar, Christine Collins, Jens Kort, Gretja Schnell, and Jill Beyer

Subjects
0301 basic medicine, Oncology, medicine.medical_specialty, Hepatology, Combination therapy, business.industry, 03 medical and health sciences, 030104 developmental biology, Internal medicine, Genotype, medicine, In patient, business, Direct acting
Published
2016

25. Characterization of resistant HIV variants generated by in vitro passage with lopinavir/ritonavir

Author

Hongmei Mo, Eugene Sun, Dale J. Kempf, Liangjun Lu, Tatyana Dekhtyar, Akhteruzzaman Molla, and Kent D. Stewart

Subjects
Models, Molecular, Human immunodeficiency virus (HIV), Lopinavir/ritonavir, Pyrimidinones, Biology, medicine.disease_cause, Lopinavir, Cell Line, HIV Protease, Serial passage, Virology, Drug Resistance, Viral, medicine, Humans, HIV Protease Inhibitor, Protease inhibitor (pharmacology), Amino Acid Sequence, Serial Passage, Pharmacology, Ritonavir, Genetic Variation, virus diseases, HIV Protease Inhibitors, In vitro, Mutation, HIV-1, Sequence Alignment, medicine.drug
Abstract

Lopinavir (LPV, formerly ABT-378) is an HIV protease inhibitor (PI) that is co-administered with a small amount of ritonavir (RTV), which greatly increases and sustains the plasma levels of LPV. Lopinavir/ritonavir (LPV/r) has shown potent antiviral activity in both therapy-nai;ve and PI-experienced patients. To assess the effect of pharmacologically relevant ratios of LPV/RTV (LPV/r) on the emergence of resistant HIV in vitro, HIV-1 pNL4-3 was passaged in the presence of increasing concentrations of LPV alone and LPV/r. Passages with fixed 5/1 and 15/1 concentration ratios of LPV/r initially selected I84V and I50V/M46I mutants, respectively. Selection with LPV alone also generated the same initial mutants (I50V/M46I) as the 15/1 LPV/r passage. Further passage produced other mutations previously found to be associated with PI-resistance. Phenotypic susceptibility to both LPV and RTV decreased with successive passages, irrespective of whether RTV was present in the selection experiment. Furthermore, in the two selection experiments that included RTV (at either 5/1 or 15/1 LPV/r ratio), the IC(50) of RTV at each passage evaluated was at least five-fold higher than the concentration of RTV employed at that passage, while the IC(50) of LPV toward the passaged virus was similar to the concentration of LPV used at that passage, indicating that the selective pressure was attributable to LPV and not RTV.

Published
2003

26. Design and synthesis of pseudo-Symmetric HIV protease inhibitors containing a novel hydroxymethylcarbonyl (HMC)-Hydrazide isostere

Author

Keith F. McDaniel, Lynn Colletti, Tooru Kimura, Yoshiaki Kiso, Tatyana Dekhtyar, Yoshio Hayashi, and Koushi Hidaka

Subjects
Stereochemistry, Isostere, medicine.medical_treatment, Clinical Biochemistry, Pharmaceutical Science, Hydrazide, Biochemistry, Chemical synthesis, Inhibitory Concentration 50, Structure-Activity Relationship, chemistry.chemical_compound, HIV Protease, Drug Discovery, medicine, Humans, Structure–activity relationship, HIV Protease Inhibitor, Protease inhibitor (pharmacology), Molecular Biology, Protease, biology, Molecular Mimicry, Organic Chemistry, HIV Protease Inhibitors, Hydrazines, chemistry, Enzyme inhibitor, Drug Design, biology.protein, Molecular Medicine, Oligopeptides
Abstract

Pseudo-symmetric HIV-1 protease inhibitors containing a novel HMC-hydrazide isostere as the transition-state mimic were designed and synthesized. Most of the synthetic compounds with varied structures at the P and P' sites around this core unit showed potent inhibitory activity against HIV-1 protease with nanomolar K(i) values.

Published
2003

27. Pooled resistance analysis in HCV genotype 1–6-infected patients treated with glecaprevir/pibrentasvir in phase 2 and 3 clinical trials

Author

Federico J. Mensa, Preethi Krishnan, Rakesh Tripathi, Thomas Reisch, Lois Larsen, Gretja Schnell, Tami Pilot-Matias, Jill Beyer, Christine Collins, Wangang Xie, Michelle Irvin, Teresa I. Ng, and Tatyana Dekhtyar

Subjects
0301 basic medicine, medicine.medical_specialty, Hepatology, business.industry, 030106 microbiology, Gastroenterology, Clinical trial, 03 medical and health sciences, 0302 clinical medicine, Hcv genotype 1, Internal medicine, Medicine, 030211 gastroenterology & hepatology, Glecaprevir / pibrentasvir, business
Published
2017

28. Resistance selection using glecaprevir and pibrentasvir in replicons of major hepatitis C virus genotypes

Author

Tatyana Dekhtyar, Thomas Reisch, L. Lu, Preethi Krishnan, Rakesh Tripathi, Gretja Schnell, Tami Pilot-Matias, Teresa I. Ng, Christine Collins, Michelle Irvin, and Jill Beyer

Subjects
Hepatology, Resistance (ecology), Hepatitis C virus, Glecaprevir, Biology, medicine.disease_cause, Virology, Pibrentasvir, 03 medical and health sciences, 0302 clinical medicine, Genotype, medicine, 030211 gastroenterology & hepatology, 030212 general & internal medicine, Replicon, Selection (genetic algorithm)
Published
2017

29. 2-Pyridyl P1'-substituted symmetry-based human immunodeficiency virus protease inhibitors (A-792611 and A-790742) with potential for convenient dosing and reduced side effects

Author

David J. Grampovnik, Lynn Colletti, Dale J. Kempf, Larry L. Klein, Mulugeta Mamo, David A. Degoey, Sue J. Swanson, Kennan C. Marsh, David Morfitt, Bach Nguyen, Tatyana Dekhtyar, Warren M. Kati, Hongmei Mo, Akhteruzzaman Molla, Clinton M. Yeung, William J. Flosi, Charles A. Flentge, Hui-Ju Chen, John T. Randolph, Vincent S. Stoll, and James M. Schmidt

Subjects
Models, Molecular, Cell Membrane Permeability, Pyridines, Rats, Gunn, Biological Availability, Hyperlipidemias, In Vitro Techniques, Crystallography, X-Ray, Structure-Activity Relationship, Dogs, HIV Protease, In vivo, Drug Discovery, Drug Resistance, Viral, Putrescine, HIV Protease Inhibitor, Potency, Animals, Humans, Protease inhibitor (pharmacology), Hyperbilirubinemia, chemistry.chemical_classification, Binding Sites, biology, Wild type, Stereoisomerism, Dipeptides, HIV Protease Inhibitors, Bioavailability, Rats, Enzyme, Biochemistry, chemistry, Enzyme inhibitor, Mutation, biology.protein, HIV-1, Microsomes, Liver, Molecular Medicine, Carbamates, Caco-2 Cells
Abstract

A series of symmetry-based HIV protease inhibitors was designed and synthesized. Modification of the core regiochemistry and stereochemistry significantly affected the potency, metabolic stability, and oral bioavailability of the inhibitors, as did the variation of a pendent arylmethyl P3 group. Optimization led to the selection of two compounds, 10c (A-790742) and 9d (A-792611), for advancement to preclinical studies. Both compounds displayed low nanomolar potency against wild type HIV in the presence of human serum, low rates of metabolism in human liver microsomes, and high oral bioavailability in animal models. The compounds were examined in a preclinical model for the hyperbilirubinemia observed with some HIV PIs, and both exhibited less bilirubin elevation than comparator compounds. X-ray crystallographic analyses of the new cores were used to examine differences in their binding modes. The antiviral activity of the compounds against protease inhibitor resistant strains of HIV was also determined.

Published
2009

30. O057 : Long-term follow-up of treatment-emergent resistance-associated variants in NS3, NS5A and NS5B with paritaprevir/r-, ombitasvir- and dasabuvir-based regimens

Author

Wangang Xie, Preethi Krishnan, Michelle Irvin, Thomas Podsadecki, Thomas Reisch, Jill Beyer, Lois Larsen, Gretja Schnell, Tatyana Dekhtyar, Tami Pilot-Matias, Christine Collins, and Rakesh Tripathi

Subjects
Pediatrics, medicine.medical_specialty, Dasabuvir, Hepatology, business.industry, Long term follow up, Ombitasvir, chemistry.chemical_compound, chemistry, Paritaprevir, Medicine, business, NS5A, medicine.drug
Published
2015

31. Identification and Structural Characterization of I84C and I84A Mutations That Are Associated with High-Level Resistance to Human Immunodeficiency Virus Protease Inhibitors and Impair Viral Replication▿

Author

Tatyana Dekhtyar, Neil Parkin, Liangjun Lu, Akhteruzzaman Molla, Dale J. Kempf, Kent D. Stewart, and Hongmei Mo

Subjects
Anti-HIV Agents, Pyridines, viruses, Atazanavir Sulfate, HIV Infections, Indinavir, Biology, Virus Replication, Antiviral Agents, Amprenavir, immune system diseases, Drug Resistance, Viral, medicine, Humans, Pharmacology (medical), Protease inhibitor (pharmacology), Saquinavir, Pharmacology, Nelfinavir, Ritonavir, virus diseases, Lopinavir, HIV Protease Inhibitors, biochemical phenomena, metabolism, and nutrition, Virology, Genes, gag, Atazanavir, Infectious Diseases, Mutation, HIV-1, Oligopeptides, medicine.drug
Abstract

Two novel human immunodeficiency virus protease mutations, I84C and I84A, were identified in patient isolates. The mutants with I84C displayed high-level resistance (median, at least 56-fold) to nelfinavir and saquinavir, but the majority remained susceptible to lopinavir. In contrast, isolates with the I84A mutation exhibited ≥33-fold median increased levels of resistance to nelfinavir, indinavir, amprenavir, ritonavir, lopinavir, saquinavir, and atazanavir. Isolates with the I84A or I84C mutation tended to be more resistant than the isolates with the I84V mutation. Modeling of the structure of the mutant proteases indicated that the I84V, I84C, and I84A mutations all create unoccupied volume in the active site, with I84A introducing the greatest change in the accessible surface area from that of the wild-type structure.

Published
2006

32. Identification and characterization of mutations conferring resistance to an HCV RNA-dependent RNA polymerase inhibitor in vitro

Author

Tatyana Dekhtyar, Akhteruzumman Molla, Liangjun Lu, Tami Pilot-Matias, Ron Pithawalla, Kent D. Stewart, Wenping He, Hongmei Mo, Gennadiy Koev, Rolf Wagner, Sherie Masse, Dan Larson, Teresa Ng, Todd D. Bosse, and Preethi Krishnan

Subjects
Models, Molecular, Genes, Viral, viruses, Hepatitis C virus, Mutant, Alpha interferon, Hepacivirus, Biology, medicine.disease_cause, Virus Replication, Virus, Cell Line, Viral Proteins, Virology, Drug Resistance, Viral, medicine, Humans, Replicon, Enzyme Inhibitors, Gene, Subgenomic mRNA, Pharmacology, virus diseases, biochemical phenomena, metabolism, and nutrition, RNA-Dependent RNA Polymerase, Molecular biology, digestive system diseases, RNA Polymerase Inhibitor, Mutation
Abstract

Compound A-837093, a non-nucleoside HCV RNA-dependent RNA polymerase inhibitor, displayed nanomolar potencies against HCV genotypes 1a and 1b replicons. It also exhibited an excellent metabolic profile and achieved high plasma and liver concentrations in animals. In order to characterize the development of resistance to this anti-HCV agent, HCV subgenomic 1b strain N replicon cells were cultured in the presence of A-837093 with G418. Mutations S368A, Y448H, G554D, Y555C, and D559G in the NS5B polymerase gene were identified that led to substantial decreases in the susceptibilities of 1b genotype replicons to the inhibitor A-837093. However, the resistant mutants remained susceptible to HCV protease inhibitor BILN-2061 and alpha interferon as well as to a different class of non-nucleoside HCV polymerase inhibitor. In addition, each single resistant mutation identified significantly reduced the replication capacity of mutant compared to wild-type replicon. These findings provide a strategic guide for the future development of non-nucleoside inhibitors of HCV NS5B polymerase.

Published
2006

33. A replicon-based shuttle vector system for assessing the phenotype of HCV NS5B polymerase genes isolated from patient populations

Author

Andrew Roth, Tatyana Dekhtyar, Akhteruzzaman Molla, Chih-Ming Chen, Tami Pilot-Matias, Gennadiy Koev, Liangjun Lu, Ben Hock Lim, Preethi Krishnan, Rubina Mondal, Warren M. Kati, Ron Pithawalla, Yupeng He, Rakesh Tripathi, Teresa I. Ng, Hongmei Mo, and Tim Middleton

Subjects
Gene Expression Regulation, Viral, Genotype, Hepatitis C virus, Population, Genetic Vectors, RNA-dependent RNA polymerase, Viral quasispecies, Hepacivirus, Biology, Viral Nonstructural Proteins, medicine.disease_cause, Antiviral Agents, chemistry.chemical_compound, Shuttle vector, Virology, RNA polymerase, Drug Resistance, Viral, medicine, Humans, Replicon, Enzyme Inhibitors, education, NS5B, education.field_of_study, RNA-Dependent RNA Polymerase, Molecular biology, Hepatitis C, Phenotype, chemistry, RNA, Viral, Plasmids
Abstract

Hepatitis C virus (HCV) replicon-based shuttle vectors that permit phenotypes of NS5B polymerase genes from a large number of patient isolates to be rapidly assessed when transiently expressed in cultured cells were designed. When used to test responses to an inhibitor of HCV RNA-dependent RNA polymerase, IC50 values for inhibition covered a several hundred-fold range among 47 patient samples tested. This observation highlights the variability that can be found by testing isolates derived from HCV-infected subjects. Partial suppression with a polymerase inhibitor of the most sensitive species permitted detection of minor quasispecies that were 7–200-fold more resistant than the bulk population in approximately half of the samples. Sequence analysis showed a wide range of amino acid changes not detected by conventional selection methods using laboratory-derived strains. This approach provides a means to assess variation in antiviral efficacy, and to predict possible responses in a clinical setting.

Published
2006

34. Antiviral interactions of an HCV polymerase inhibitor with an HCV protease inhibitor or interferon in vitro

Author

Teresa I. Ng, C. Thomas Lin, Gennadiy Koev, Lixin Han, Ping Yan, Hongmei Mo, Akhteruzzaman Molla, and Tatyana Dekhtyar

Subjects
Macrocyclic Compounds, Serine Proteinase Inhibitors, viruses, Hepatitis C virus, Hepacivirus, Microbial Sensitivity Tests, Biology, medicine.disease_cause, Antiviral Agents, Virus, Cell Line, chemistry.chemical_compound, Inhibitory Concentration 50, Interferon, Virology, medicine, Humans, Protease inhibitor (pharmacology), Replicon, Enzyme Inhibitors, NS5B, Polymerase, Pharmacology, RNA, Interferon-alpha, Drug Synergism, RNA-Dependent RNA Polymerase, Thiazoles, chemistry, biology.protein, Quinolines, Carbamates, medicine.drug
Abstract

The combinations of Abbott Hepatitis C virus (HCV) polymerase A-782759 with either Boehringer Ingelheim HCV NS3 protease inhibitor BILN-2061 or interferon (IFN) displayed additive to synergistic relationships over a range of concentrations of two-drug combination. Treatment of HCV replicon with A-782759, IFN or BILN-2061 for about 16 days resulted in dramatic reductions in HCV RNA (5.1, 3.0 and 3.9 log10 RNA copies, respectively). However, none of the compounds tested alone lead to replicon RNA reduction to undetectable levels. Ongoing replication in the presence of A-782759 or BILN-2061 was associated with the appearance of resistant mutations M414T in NS5B and D168V in NS3, respectively. In contrast, a combination of A-782759 with BILN-2061 resulted in greater than 7 logs RNA reduction leading to undetectable replicon RNA after 16 days of treatment. Our findings suggest that a monotherapy with either drug alone is likely to result in development of resistant mutants. However, a combination therapy with polymerase inhibitor has the potential to improve the efficacy of IFN or a protease inhibitor alone in vivo, due to the lower likelihood of resistance development.

Published
2006

35. Synthesis, antiviral activity, and pharmacokinetic evaluation of P3 pyridylmethyl analogs of oximinoarylsulfonyl HIV-1 protease inhibitors

Author

Tatyana Dekhtyar, Mingua Sun, John T. Randolph, Chen Zhao, Larry L. Klein, Hongmei Mo, Dale J. Kempf, Warren M. Kati, Charles A. Flentge, William J. Flosi, Lynn Colletti, Clinton M. Yeung, Peggy P. Huang, Akhteruzzaman Molla, David A. Degoey, and Kennan C. Marsh

Subjects
Anti-HIV Agents, Pyridines, Clinical Biochemistry, Molecular Conformation, Pharmaceutical Science, Microbial Sensitivity Tests, Pharmacology, Biochemistry, Chemical synthesis, Structure-Activity Relationship, Dogs, Pharmacokinetics, HIV-1 protease, In vivo, Drug Discovery, medicine, Animals, Humans, Protease inhibitor (pharmacology), Molecular Biology, Sulfonamides, biology, Chemistry, Organic Chemistry, Stereoisomerism, HIV Protease Inhibitors, Bioavailability, Rats, Enzyme inhibitor, Area Under Curve, Drug Design, biology.protein, HIV-1, Molecular Medicine, Cytochrome P-450 CYP3A Inhibitors, Ritonavir, medicine.drug
Abstract

As a continuation of the recently communicated discovery of oximinoarylsulfonamides as potent inhibitors of HIV-1 aspartyl protease, compounds bearing pyridylmethyl substituents at P3 were designed and synthesized. Potent analogs in this series provided low single-digit nanomolar EC50 values against both wild-type HIV and resistant mutant virus (A17), attenuated some 3- to 12-fold in the presence of 50% human serum. Pharmacokinetic results for compounds in this series showed good to excellent exposure when co-administered orally with an equal amount of ritonavir (5mg/kg each) in the rat, with average AUC8 microg h/mL. Similar dosing in dog resulted in significantly lower plasma levels (average AUC2 microg h/mL). The 3-pyridylmethyl analog 30 gave the best overall exposure (rat AUC=7.1 microg h/mL and dog AUC=4.9 microg h/mL), however, this compound was found to be a potent inhibitor of cytochrome P450 3A (Ki=2.4 nM).

Published
2005

36. Oximinoarylsulfonamides as potent HIV protease inhibitors

Author

Tatyana Dekhtyar, Chen Zhao, Dale J. Kempf, Minghua Sun, Larry L. Klein, Clinton M. Yeung, Charles A. Flentge, Vincent S. Stoll, and John T. Randolph

Subjects
Models, Molecular, Clinical Biochemistry, Molecular Conformation, Pharmaceutical Science, Pyrimidinones, Biochemistry, Lopinavir, Amprenavir, HIV Protease, Drug Discovery, medicine, HIV Protease Inhibitor, Protease inhibitor (pharmacology), Furans, Molecular Biology, chemistry.chemical_classification, Sulfonamides, Binding Sites, Ritonavir, biology, Chemistry, Organic Chemistry, virus diseases, HIV Protease Inhibitors, Virology, Kinetics, Enzyme, Enzyme inhibitor, Drug Design, biology.protein, Molecular Medicine, Carbamates, Pharmacophore, medicine.drug
Abstract

The need for a potent HIV protease inhibitor (PI) to combat emerging PI-resistant viruses is anticipated. Analogs formulated from the combination of structural fragments of Ritonavir, Lopinavir, and Amprenavir were synthesized. Analogs containing the oxime pharmacophore were found to have improved activities against both wild type and resistant (A17) viruses. The synthesis and structure-activity relationships (SAR) based upon the in vitro IC50 of this series of compounds are reported.

Published
2005

37. Conserved residues in the coiled-coil pocket of human immunodeficiency virus type 1 gp41 are essential for viral replication and interhelical interaction

Author

Akhteruzzaman Molla, Kent D. Stewart, Kerry M. Swift, Edmund D. Matayoshi, Teresa Ng, Tatyana Dekhtyar, Alex K. Konstantinidis, Warren M. Kati, William E. Kohlbrenner, and Hongmei Mo

Subjects
Models, Molecular, Mutant, Interhelical interaction, Molecular Sequence Data, Fluorescence Polarization, Biology, Gp41, Virus Replication, Structure-Activity Relationship, Virology, Viral replication, Biomarkers, Tumor, Humans, Point Mutation, Coiled-coil, Amino Acid Sequence, Peptide sequence, Cell Line, Transformed, Coiled coil, Infectivity, C-Peptide, Point mutation, Tumor Suppressor Proteins, Wild type, HIV Envelope Protein gp41, Cell biology, DNA-Binding Proteins, Biochemistry, Phosphopyruvate Hydratase, HIV-1
Abstract

The human immunodeficiency virus type 1 (HIV-1) gp41 plays an important role in mediating the fusion of HIV with host cells. During the fusion process, three N-terminal helices and three C-terminal helices pack in an anti-parallel direction to form a six-helix bundle. X-ray crystallographic analysis of the gp41 core demonstrated that within each coiled-coil interface, there is a deep and large pocket, formed by a cluster of residues in the N-helix coiled-coil. In this report, we systematically analyzed the role of seven conserved residues that are either lining or packing this pocket on the infectivity and interhelical interaction using novel approaches. Our results show that residues L568, V570, W571, and K574 of the N-helix that are lining the side chain and right wall of the pocket are important for establishing a productive infection. Mutations V570A and W571A completely abolished replication, while replication of the L568A and K574A mutants was significantly attenuated relative to wild type. Similarly, residues W628, W631, and I635 of the C-helix that insert into the pocket are essential for infectivity. The impaired infectivity of these seven mutants is in part attributed to the loss in binding affinity of the interhelical interaction. Molecular modeling of the crystal structure of the coiled-coil further shows that alanine substitution of those residues disrupts the hydrophobic interaction between the N- and C-helix. These results suggest that the conserved residues in the coiled-coil domain play a key role in HIV infection and this coiled-coil pocket is a good target for development of inhibitors against HIV. In addition, our data indicate that the novel fluorescence polarization assay described in this study could be valuable in screening for inhibitors that block the interhelical interaction and HIV entry.

Published
2004

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