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1. Woolly Monkey–HBV Infection in Squirrel Monkeys as a Surrogate Nonhuman Primate Model of HBV Infection

Author

Christopher Y. Chen, Benjamin Y. Winer, Deborah Chavez, Bernadette Guerra, Kathleen M. Brasky, Stacey Eng, Eduardo Salas, Danny Tam, Joe H. Simmons, Christian R. Abee, William E. Delaney, Alexander Ploss, Robert E. Lanford, and Christian Voitenleitner

Subjects
Diseases of the digestive system. Gastroenterology, RC799-869
Abstract

Development of curative therapies for chronic hepatitis B virus (HBV) infection will likely require new animal models. Here, we evaluate HBV infection in squirrel monkeys based on the high‐sequence homology of the HBV receptor, Na+/taurocholate co‐transporting peptide (NTCP), between humans and squirrel monkeys. HBV PreS1 peptide was examined for binding human and squirrel monkey NTCP. Immunodeficient Fah−/−, NOD, Rag1−/−, Il2Rgnull (FNRG) mice engrafted with human or squirrel monkey hepatocytes were challenged with HBV or Woolly Monkey HBV (WMHBV). In addition, adult squirrel monkeys were inoculated with HBV, WMHBV, adeno‐associated virus containing an infectious genome of HBV (AAV‐HBV), and AAV‐WMHBV. Finally, neonate squirrel monkeys were assessed for the potential of chronic infection with WMHBV. PreS1 peptide efficiently bound to human and squirrel monkey NTCP but not to mouse or capuchin NTCP. FNRG mice engrafted with squirrel monkey hepatocytes were susceptible to infection by WMHBV but not human HBV. Similarly, adult squirrel monkeys could be infected with WMHBV but not human HBV, whereas chimeric mice engrafted with human hepatocytes were susceptible to HBV but not WMHBV. Infection of squirrel monkeys with AAV‐WMHBV yielded maximum viremia of 108 genomes/mL with detectable virus for up to 8 months. Notably, covalently closed circular DNA was detected in the liver of these animals. Infection of neonates with WMHBV led to detectable viremia for up to 6 months. Conclusions: Adult and neonate squirrel monkeys exhibited prolonged WMHBV viremia lasting 6‐8 months. This is greater than twice the duration of viremia achieved in other nonhuman primates and suggests that squirrel monkeys may be a suitable model for testing HBV therapeutics.

Published
2020
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2. Hepatitis C genotype 1a replicon improved through introduction of fitness mutations

Author

Christian Voitenleitner, Jill Bechtel, Ann Arfsten, and Robert Hamatake

Subjects
Hepatitis C, genotype 1a replicon, fitness, transient assay, Biology (General), QH301-705.5
Abstract

The use of subgenomic replicon systems has long been a valuable screening tool for the discovery of small molecule antivirals against Hepatitis C virus. While genotype 1a replicon systems have been widely used in stable systems, use in transient assays has been hampered by low signal. Here we describe the generation of a more robust genotype 1a (H77) replicon through the introduction of two fitness mutations, NS4A-K1691R and NS4B-E1726G, for use in transient transfections. While these mutations significantly improved the signal to noise ratio, leading to more robust data, they have no effect on the potency of tool compounds against various targets of HCV, thereby making this new system a powerful tool for screening of compounds against the genotype 1a replicon.

Published
2012
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3. Toll‐Like Receptor 8 Agonist GS‐9688 Induces Sustained Efficacy in the Woodchuck Model of Chronic Hepatitis B

Author

Ricardo Ramirez, Li Li, William E. Delaney, Stephan Menne, Sarina Ma, Changsuek Yon, Don Kang, Jason Chamberlain, Christian Voitenleitner, William Rowe, Ruth Chu, Dhivya Ramakrishnan, Magdeleine Hung, Manasa Suresh, Divya Pattabiraman, Stephane Daffis, Paul J. Cote, Rex Santos, Bei Li, Simon P. Fletcher, Scott Balsitis, Sandra Spurlock, Mish Michael R, Jim Zheng, and Richard L. Mackman

Subjects
0301 basic medicine, Agonist, medicine.drug_class, Viral Hepatitis, viruses, Pharmacology, Virus Replication, medicine.disease_cause, Antiviral Agents, 03 medical and health sciences, Hepatitis B, Chronic, 0302 clinical medicine, Immune system, Antigen, medicine, Animals, Hepatitis B Virus, Woodchuck, Humans, Hepatitis Antibodies, Hepatitis B virus, Hepatology, biology, business.industry, Woodchuck hepatitis virus, Hepatitis Antigens, Original Articles, biochemical phenomena, metabolism, and nutrition, Hepatitis B, biology.organism_classification, medicine.disease, digestive system diseases, Disease Models, Animal, Pyrimidines, 030104 developmental biology, Toll-Like Receptor 8, Marmota, DNA, Viral, biology.protein, Original Article, 030211 gastroenterology & hepatology, Antibody, Hexanols, business, Viral load
Abstract

Background and aims GS-9688 (selgantolimod) is an oral selective small molecule agonist of toll-like receptor 8 in clinical development for the treatment of chronic hepatitis B. In this study, we evaluated the antiviral efficacy of GS-9688 in woodchucks chronically infected with woodchuck hepatitis virus (WHV), a hepadnavirus closely related to hepatitis B virus. Approach and results WHV-infected woodchucks received eight weekly oral doses of vehicle, 1 mg/kg GS-9688, or 3 mg/kg GS-9688. Vehicle and 1 mg/kg GS-9688 had no antiviral effect, whereas 3 mg/kg GS-9688 induced a >5 log10 reduction in serum viral load and reduced WHV surface antigen (WHsAg) levels to below the limit of detection in half of the treated woodchucks. In these animals, the antiviral response was maintained until the end of the study (>5 months after the end of treatment). GS-9688 treatment reduced intrahepatic WHV RNA and DNA levels by >95% in animals in which the antiviral response was sustained after treatment cessation, and these woodchucks also developed detectable anti-WHsAg antibodies. The antiviral efficacy of weekly oral dosing with 3 mg/kg GS-9688 was confirmed in a second woodchuck study. The antiviral response to GS-9688 did not correlate with systemic GS-9688 or cytokine levels but was associated with transient elevation of liver injury biomarkers and enhanced proliferative response of peripheral blood mononuclear cells to WHV peptides. Transcriptomic analysis of liver biopsies taken prior to treatment suggested that T follicular helper cells and various other immune cell subsets may play a role in the antiviral response to GS-9688. Conclusions Finite, short-duration treatment with a clinically relevant dose of GS-9688 is well tolerated and can induce a sustained antiviral response in WHV-infected woodchucks; the identification of a baseline intrahepatic transcriptional signature associated with response to GS-9688 treatment provides insights into the immune mechanisms that mediate this antiviral effect.

Published
2020

4. Woolly Monkey–HBV Infection in Squirrel Monkeys as a Surrogate Nonhuman Primate Model of HBV Infection

Author

Benjamin Y. Winer, Kathleen M. Brasky, Robert E. Lanford, Christian R. Abee, William E. Delaney, Alexander Ploss, Deborah Chavez, Joe H. Simmons, Danny Tam, Christopher Y. Chen, Christian Voitenleitner, Eduardo Salas, Bernadette Guerra, and Stacey Eng

Subjects
animal diseases, viruses, Viremia, Nod, behavioral disciplines and activities, Woolly monkey, Recombination-activating gene, Virus, 03 medical and health sciences, 0302 clinical medicine, medicine, lcsh:RC799-869, Receptor, 030304 developmental biology, 0303 health sciences, Hepatology, biology, Squirrel monkey, virus diseases, Original Articles, biology.organism_classification, medicine.disease, Virology, digestive system diseases, 3. Good health, Chronic infection, 030211 gastroenterology & hepatology, lcsh:Diseases of the digestive system. Gastroenterology, Original Article
Abstract

Development of curative therapies for chronic hepatitis B virus (HBV) infection will likely require new animal models. Here, we evaluate HBV infection in squirrel monkeys based on the high-sequence homology of the HBV receptor, Na+/taurocholate co-transporting peptide (NTCP), between humans and squirrel monkeys. HBV PreS1 peptide was examined for binding human and squirrel monkey NTCP. Immunodeficient Fah -/- , NOD, Rag1 -/- , Il2Rg null (FNRG) mice engrafted with human or squirrel monkey hepatocytes were challenged with HBV or Woolly Monkey HBV (WMHBV). In addition, adult squirrel monkeys were inoculated with HBV, WMHBV, adeno-associated virus containing an infectious genome of HBV (AAV-HBV), and AAV-WMHBV. Finally, neonate squirrel monkeys were assessed for the potential of chronic infection with WMHBV. PreS1 peptide efficiently bound to human and squirrel monkey NTCP but not to mouse or capuchin NTCP. FNRG mice engrafted with squirrel monkey hepatocytes were susceptible to infection by WMHBV but not human HBV. Similarly, adult squirrel monkeys could be infected with WMHBV but not human HBV, whereas chimeric mice engrafted with human hepatocytes were susceptible to HBV but not WMHBV. Infection of squirrel monkeys with AAV-WMHBV yielded maximum viremia of 108 genomes/mL with detectable virus for up to 8 months. Notably, covalently closed circular DNA was detected in the liver of these animals. Infection of neonates with WMHBV led to detectable viremia for up to 6 months. Conclusions: Adult and neonate squirrel monkeys exhibited prolonged WMHBV viremia lasting 6-8 months. This is greater than twice the duration of viremia achieved in other nonhuman primates and suggests that squirrel monkeys may be a suitable model for testing HBV therapeutics.

Published
2020

5. Design of N-Benzoxaborole Benzofuran GSK8175—Optimization of Human Pharmacokinetics Inspired by Metabolites of a Failed Clinical HCV Inhibitor

Author

Christian Voitenleitner, Huichang Zhang, Renae M. Crosby, Kirsten M. Kahler, Feng Wang, John F. Miller, Elizabeth M. Turner, Daniel J. Price, Jing Fang, Andrew Maynard, Vincent W.-F. Tai, Katrina L. Creech, Andrew J. Peat, J. Brad Shotwell, Shawn P. Williams, Amanda Mathis, Jeffrey J. Pouliot, and Pek Yoke Chong

Subjects
Viral protein, Hepatitis C virus, Hepacivirus, Pharmacology, Crystallography, X-Ray, medicine.disease_cause, Antiviral Agents, 01 natural sciences, Mice, 03 medical and health sciences, chemistry.chemical_compound, Dogs, Pharmacokinetics, In vivo, Drug Discovery, medicine, Animals, Humans, Benzofuran, NS5B, Polymerase, Nucleic Acid Synthesis Inhibitors, 030304 developmental biology, 0303 health sciences, Molecular Structure, biology, Boronic Acids, Rats, 0104 chemical sciences, Macaca fascicularis, 010404 medicinal & biomolecular chemistry, chemistry, Drug Design, biology.protein, Molecular Medicine, Boronic acid, Half-Life
Abstract

[Image: see text] We previously described the discovery of GSK5852 (1), a non-nucleoside polymerase (NS5B) inhibitor of hepatitis C virus (HCV), in which an N-benzyl boronic acid was essential for potent antiviral activity. Unfortunately, facile benzylic oxidation resulted in a short plasma half-life (5 h) in human volunteers, and a backup program was initiated to remove metabolic liabilities associated with 1. Herein, we describe second-generation NS5B inhibitors including GSK8175 (49), a sulfonamide-N-benzoxaborole analog with low in vivo clearance across preclinical species and broad-spectrum activity against HCV replicons. An X-ray structure of NS5B protein cocrystallized with 49 revealed unique protein-inhibitor interactions mediated by an extensive network of ordered water molecules and the first evidence of boronate complex formation within the binding pocket. In clinical studies, 49 displayed a 60–63 h half-life and a robust decrease in viral RNA levels in HCV-infected patients, thereby validating our hypothesis that reducing benzylic oxidation would improve human pharmacokinetics and lower efficacious doses relative to 1.

Published
2019

7. Spatiotemporal Analysis of Hepatitis B Virus X Protein in Primary Human Hepatocytes

Author

Hyock Joo Kwon, Christian Voitenleitner, Weimei Xing, Dmytro Kornyeyev, Simon P. Fletcher, Magdeleine Hung, Christine M. Livingston, Dhivya Ramakrishnan, and Rudolf K. F. Beran

Subjects
Gene Expression Regulation, Viral, Small interfering RNA, Hepatitis B virus, Viral protein, viruses, Immunology, Fluorescent Antibody Technique, Gene Expression, Enzyme-Linked Immunosorbent Assay, DDB1, medicine.disease_cause, Microbiology, 03 medical and health sciences, 0302 clinical medicine, Virology, medicine, Gene silencing, Humans, Viral Regulatory and Accessory Proteins, Amino Acid Sequence, Spotlight, 030304 developmental biology, 0303 health sciences, biology, Smc5/6 complex, Antibodies, Monoclonal, Hepatitis B, digestive system diseases, Ubiquitin ligase, Cell biology, Virus-Cell Interactions, DNA-Binding Proteins, HBx, Protein Transport, Insect Science, Host-Pathogen Interactions, biology.protein, Hepatocytes, Trans-Activators, 030211 gastroenterology & hepatology, Peptides, Nuclear localization sequence, Protein Binding
Abstract

Hepatitis B virus X protein (HBx) is a promising drug target since it promotes the degradation of the host structural maintenance of chromosomes 5/6 complex (Smc5/6) that inhibits HBV transcription. To date, it has not been possible to study HBx in physiologically relevant cell culture systems due to the lack of a highly specific and selective HBx antibody. In this study, we developed a novel monoclonal HBx antibody and performed a spatiotemporal analysis of HBx in a natural infection system. This revealed that HBx localizes to the nucleus of infected cells, is expressed shortly after infection, and has a short half-life. In addition, we demonstrated that inhibiting HBx expression or function promotes the reappearance of Smc6 in the nucleus of infected cells. These data provide new insights into HBx and underscore its potential as a novel target for the treatment of chronic HBV infection., The structural maintenance of chromosomes 5/6 complex (Smc5/6) is a host restriction factor that suppresses hepatitis B virus (HBV) transcription. HBV counters this restriction by expressing the X protein (HBx), which redirects the host DNA damage-binding protein 1 (DDB1) E3 ubiquitin ligase to target Smc5/6 for degradation. HBx is an attractive therapeutic target for the treatment of chronic hepatitis B (CHB), but it is challenging to study this important viral protein in the context of natural infection due to the lack of a highly specific and sensitive HBx antibody. In this study, we developed a novel monoclonal antibody that enables detection of HBx protein in HBV-infected primary human hepatocytes (PHH) by Western blotting and immunofluorescence. Confocal imaging studies with this antibody demonstrated that HBx is predominantly located in the nucleus of HBV-infected PHH, where it exhibits a diffuse staining pattern. In contrast, a DDB1-binding-deficient HBx mutant was detected in both the cytoplasm and nucleus, suggesting that the DDB1 interaction plays an important role in the nuclear localization of HBx. Our study also revealed that HBx is expressed early after infection and has a short half-life (∼3 h) in HBV-infected PHH. In addition, we found that treatment with small interfering RNAs (siRNAs) that target DDB1 or HBx mRNA decreased HBx protein levels and led to the reappearance of Smc6 in the nuclei of HBV-infected PHH. Collectively, these studies provide the first spatiotemporal analysis of HBx in a natural infection system and also suggest that HBV transcriptional silencing by Smc5/6 can be restored by therapeutic targeting of HBx. IMPORTANCE Hepatitis B virus X protein (HBx) is a promising drug target since it promotes the degradation of the host structural maintenance of chromosomes 5/6 complex (Smc5/6) that inhibits HBV transcription. To date, it has not been possible to study HBx in physiologically relevant cell culture systems due to the lack of a highly specific and selective HBx antibody. In this study, we developed a novel monoclonal HBx antibody and performed a spatiotemporal analysis of HBx in a natural infection system. This revealed that HBx localizes to the nucleus of infected cells, is expressed shortly after infection, and has a short half-life. In addition, we demonstrated that inhibiting HBx expression or function promotes the reappearance of Smc6 in the nucleus of infected cells. These data provide new insights into HBx and underscore its potential as a novel target for the treatment of chronic HBV infection.

Published
2019

8. Cell-Free Hepatitis B Virus Capsid Assembly Dependent on the Core Protein C-Terminal Domain and Regulated by Phosphorylation

Author

Nicholas T. Streck, Kuancheng Liu, Laurie Luckenbaugh, Laurie Ludgate, Jianming Hu, Christian Voitenleitner, William E. Delaney, and Stacey Eng

Subjects
Gene Expression Regulation, Viral, 0301 basic medicine, Hepatitis B virus, Reticulocytes, viruses, Immunology, Protein domain, Biology, Virus Replication, medicine.disease_cause, Microbiology, Cell-free system, 03 medical and health sciences, Capsid, Protein Domains, Virology, medicine, Animals, Humans, Phosphorylation, Cell-Free System, Viral Core Proteins, Virus Assembly, Structure and Assembly, C-terminus, virus diseases, RNA, Hepatitis B Core Antigens, digestive system diseases, 030104 developmental biology, Viral replication, Insect Science, Host-Pathogen Interactions, RNA, Viral, Capsid Proteins, Rabbits
Abstract

Multiple subunits of the hepatitis B virus (HBV) core protein (HBc) assemble into an icosahedral capsid that packages the viral pregenomic RNA (pgRNA). The N-terminal domain (NTD) of HBc is sufficient for capsid assembly, in the absence of pgRNA or any other viral or host factors, under conditions of high HBc and/or salt concentrations. The C-terminal domain (CTD) is deemed dispensable for capsid assembly although it is essential for pgRNA packaging. We report here that HBc expressed in a mammalian cell lysate, rabbit reticulocyte lysate (RRL), was able to assemble into capsids when (low-nanomolar) HBc concentrations mimicked those achieved under conditions of viral replication in vivo and were far below those used previously for capsid assembly in vitro . Furthermore, at physiologically low HBc concentrations in RRL, the NTD was insufficient for capsid assembly and the CTD was also required. The CTD likely facilitated assembly under these conditions via RNA binding and protein-protein interactions. Moreover, the CTD underwent phosphorylation and dephosphorylation events in RRL similar to those seen in vivo which regulated capsid assembly. Importantly, the NTD alone also failed to accumulate in mammalian cells, likely resulting from its failure to assemble efficiently. Coexpression of the full-length HBc rescued NTD assembly in RRL as well as NTD expression and assembly in mammalian cells, resulting in the formation of mosaic capsids containing both full-length HBc and the NTD. These results have important implications for HBV assembly during replication and provide a facile cell-free system to study capsid assembly under physiologically relevant conditions, including its modulation by host factors. IMPORTANCE Hepatitis B virus (HBV) is an important global human pathogen and the main cause of liver cancer worldwide. An essential component of HBV is the spherical capsid composed of multiple copies of a single protein, the core protein (HBc). We have developed a mammalian cell-free system in which HBc is expressed at physiological (low) concentrations and assembles into capsids under near-physiological conditions. In this cell-free system, as in mammalian cells, capsid assembly depends on the C-terminal domain (CTD) of HBc, in contrast to other assembly systems in which HBc assembles into capsids independently of the CTD under conditions of nonphysiological protein and salt concentrations. Furthermore, the phosphorylation state of the CTD regulates capsid assembly and RNA encapsidation in the cell-free system in a manner similar to that seen in mammalian cells. This system will facilitate detailed studies on capsid assembly and RNA encapsidation under physiological conditions and identification of antiviral agents that target HBc.

Published
2016

9. Nucleotide Prodrug Containing a Nonproteinogenic Amino Acid To Improve Oral Delivery of a Hepatitis C Virus Treatment

Author

Stacey Eng, Thorsten A. Kirschberg, Darius Babusis, Christian Voitenleitner, Gabriel Birkus, Ting Wang, Yili Xu, Neeraj Tirunagari, Huiling Yang, Martijn Fenaux, Joy Y. Feng, Yeojin Park, Aesop Cho, and Adrian S. Ray

Subjects
0301 basic medicine, nucleotide prodrug, Male, cathepsin A, Adenosine, 030106 microbiology, Administration, Oral, Hepacivirus, Pharmacology, Virus Replication, Antiviral Agents, 03 medical and health sciences, chemistry.chemical_compound, Dogs, Oral administration, Animals, Humans, Pharmacology (medical), Nucleotide, Prodrugs, carboxyl esterase 1, Cells, Cultured, chemistry.chemical_classification, Alanine, Chemistry, Nucleotides, Triazines, Phosphoramidate, Prodrug, antiviral, Hepatitis C, Amino acid, Rats, 030104 developmental biology, Infectious Diseases, GS-6620, HCV, Nucleoside triphosphate, GS2, Efflux, Caco-2 Cells, Nucleoside, carboxyl esterase
Abstract

Delivery of pharmacologically active nucleoside triphosphate analogs to sites of viral infection is challenging. In prior work we identified a 2′-C-methyl-1′-cyano-7-deaza-adenosine C-nucleotide analog with desirable selectivity and potency for the treatment of hepatitis C virus (HCV) infection., Delivery of pharmacologically active nucleoside triphosphate analogs to sites of viral infection is challenging. In prior work we identified a 2′-C-methyl-1′-cyano-7-deaza-adenosine C-nucleotide analog with desirable selectivity and potency for the treatment of hepatitis C virus (HCV) infection. However, the prodrug selected for clinical development, GS-6620, required a high dose for meaningful efficacy and had unacceptable variability due to poor oral absorption as a result of suboptimal solubility, intestinal metabolism, and efflux transport. While obtaining clinical proof of concept for the nucleotide analog, a more effective prodrug strategy would be necessary for clinical utility. Here, we report an alternative prodrug of the same nucleoside analog identified to address liabilities of GS-6620. A phosphoramidate prodrug containing the nonproteinogenic amino acid methylalanine, an isopropyl ester and phenol in the (S) conformation at phosphorous, GS2, was found to have improved solubility, intestinal stability, and hepatic activation. GS2 is a more selective substrate for hepatically expressed carboxyl esterase 1 (CES1) and is resistant to hydrolysis by more widely expressed hydrolases, including cathepsin A (CatA) and CES2. Unlike GS-6620, GS2 was not cleaved by intestinally expressed CES2 and, as a result, was stable in intestinal extracts. Levels of liver triphosphate following oral administration of GS2 in animals were higher than those of GS-6620, even when administered under optimal conditions for GS-6620 absorption. Combined, these properties suggest that GS2 will have better oral absorption in the clinic when administered in a solid dosage form and the potential to extend the clinical proof of concept obtained with GS-6620.

Published
2018

10. Clinical and In Vitro Resistance to GS-9669, a Thumb Site II Nonnucleoside Inhibitor of the Hepatitis C Virus NS5B Polymerase

Author

Evguenia S. Svarovskaia, Hadas Dvory-Sobol, Eric Mabery, Taylor Skurnac, William E. Delaney, Eric Lawitz, John G. McHutchison, Hongmei Mo, Michael D. Miller, and Christian Voitenleitner

Subjects
Adult, Male, Sofosbuvir, Hepacivirus, Hepatitis C virus, Molecular Sequence Data, Microbial Sensitivity Tests, Thiophenes, Viral Nonstructural Proteins, medicine.disease_cause, Antiviral Agents, Cell Line, chemistry.chemical_compound, Drug Resistance, Viral, Ribavirin, Genotype, Uridine monophosphate, medicine, Humans, Pharmacology (medical), Furans, NS5B, Polymerase, Pharmacology, Fluorenes, Base Sequence, biology, Sequence Analysis, RNA, Genetic Variation, Hepatitis C, Chronic, biology.organism_classification, Virology, digestive system diseases, Treatment Outcome, Infectious Diseases, chemistry, Quinolines, biology.protein, Benzimidazoles, Female, Uridine Monophosphate, Protein Binding, medicine.drug
Abstract

Treatment with GS-9669, a novel nonnucleoside inhibitor (site II) of hepatitis C virus (HCV) nonstructural 5B (NS5B) polymerase, resulted in significant antiviral activity in HCV genotype (GT) 1 patients dosed at 50 and 500 mg once daily (QD) and at 50, 100, and 500 mg twice daily (BID) for 3 days. This report characterizes the virologic resistance to GS-9669 in vitro and in GT1 HCV-infected patients from a phase I clinical study. An in vitro resistance selection study with GS-9669 revealed substitutions at several NS5B residues that conferred resistance. The M423 variants were selected at low drug concentrations (5× the 50% effective concentration [EC 50 ]), and the L419, R422, and I482 variants were selected at higher drug concentrations (20× the EC 50 ). During the phase I clinical study, substitutions at NS5B residues 419, 422, and 486 were the predominant changes associated with GS-9669 monotherapy. Substitutions at position 423 were observed only in GT1a patients in the low-dose groups (50 and 100 mg BID). Interestingly, four HCV patients had substitutions at position 423 at baseline. Consistent with the low resistance level at this position, three patients with M423I or M423V at baseline achieved >2-log 10 reductions of HCV RNA when treated with 100 mg BID or with 500 mg QD or BID of GS-9669. The fourth patient, who had the M423V substitution at baseline, had a 4.4-log 10 reduction of HCV RNA with 500 mg BID of GS-9669. Phenotypic analyses demonstrated that the viral isolates with multiple GS-9669 resistance-associated variants have reduced susceptibility to GS-9669 and lomibuvir (VX-222) but are not cross-resistant to other classes of HCV inhibitors. (This study has been registered at ClinicalTrials.gov under registration no. NCT01431898.)

Published
2014

11. A randomized, double blind, dose escalation, first time in human study to assess the safety, tolerability, pharmacokinetics, and antiviral activity of single doses of GSK2485852 in chronically infected hepatitis C subjects

Author

Jianjun Gan, Lou Yu, David A. Wilfret, Brad Shotwell, Jill Walker, Kimberly K. Adkison, Christian Voitenleitner, Daniel J. Lee, J. Kim, Sharon Baptiste-Brown, Mark Lovern, Amanda Mathis, Andrew Spaltenstein, and Lee Moss

Subjects
business.industry, Hepatitis C virus, Cmax, Area under the curve, Pharmaceutical Science, Hepatitis C, Pharmacology, medicine.disease_cause, medicine.disease, Placebo, Interleukin 28B, Pharmacokinetics, Tolerability, Medicine, Pharmacology (medical), business
Abstract

This first-time-in-human, randomized, double-blind, placebo-controlled, dose-escalation study assessed the safety, tolerability, pharmacokinetics, and antiviral activity of GSK2485852, a hepatitis C virus (HCV) NS5B inhibitor, in 27 chronically infected HCV genotype-1 subjects. Subjects received GSK2485852 70, 420, and 70 mg with a moderate fat/caloric meal. Safety, pharmacokinetics, antiviral activity, HCV genotype/phenotype, and interleukin 28B genotype were evaluated. A statistically significant reduction in HCV ribonucleic acid (RNA) was observed after a single dose of 420 mg GSK2485852 (−1.33 log10 IU/mL) compared with placebo (−0.09 log10 IU/mL) at 24 hours post-dose. Subjects receiving 70 mg GSK2485852 were exposed to concentrations above the protein-adjusted 90% effective concentration for a short time; none experienced a significant decline in HCV RNA (−0.47 log10 copies/mL). GSK2485852 was readily absorbed; however, the observed geometric mean maximum plasma concentration (Cmax) and area under the curve (AUC) values were significantly lower than expected due to a higher-than-predicted-oral clearance. Co-administration with food reduced the AUC and Cmax of GSK2485852 by 40% and 70%, respectively. Two metabolites were detected in human blood with one having approximately 50% higher concentrations than those of the parent. GSK2485852 was well-tolerated and exhibited antiviral activity after a single 420 mg dose in HCV subjects.

Published
2014

12. In Vitro Characterization of GSK2485852, a Novel Hepatitis C Virus Polymerase Inhibitor

Author

Jill Walker, Renae M. Crosby, Jessica Vamathevan, Ermias Woldu, John Johnson, J. Brad Shotwell, Shihyun You, Stephanie Van Horn, Zhi Hong, Robert Hamatake, Amy Wang, Joseph Horton, Christian Voitenleitner, Katja Remlinger, and Katrina L. Creech

Subjects
Genotype, viruses, Hepatitis C virus, Hepacivirus, Population, Microbial Sensitivity Tests, Drug resistance, Viral Nonstructural Proteins, medicine.disease_cause, Antiviral Agents, Cell Line, chemistry.chemical_compound, RNA polymerase, Drug Resistance, Viral, medicine, Humans, Pharmacology (medical), Replicon, Enzyme Inhibitors, education, NS5B, Benzofurans, Enzyme Assays, Pharmacology, Sulfonamides, education.field_of_study, biology, High-Throughput Nucleotide Sequencing, virus diseases, Hepatitis C, Chronic, biochemical phenomena, metabolism, and nutrition, biology.organism_classification, Boronic Acids, Virology, Molecular biology, digestive system diseases, Molecular Typing, Kinetics, Infectious Diseases, chemistry, Mutation, Hepatocytes
Abstract

GSK2485852 (referred to here as GSK5852) is a hepatitis C virus (HCV) NS5B polymerase inhibitor with 50% effective concentrations (EC 50 s) in the low nanomolar range in the genotype 1 and 2 subgenomic replicon system as well as the infectious HCV cell culture system. We have characterized the antiviral activity of GSK5852 using chimeric replicon systems with NS5B genes from additional genotypes as well as NS5B sequences from clinical isolates of patients infected with HCV of genotypes 1a and 1b. The inhibitory activity of GSK5852 remained unchanged in these intergenotypic and intragenotypic replicon systems. GSK5852 furthermore displays an excellent resistance profile and shows a

Published
2013

13. Discovery of a Potent Boronic Acid Derived Inhibitor of the HCV RNA-Dependent RNA Polymerase

Author

Andrew Maynard, Renae M. Crosby, Byron Ellis, Robert Hamatake, Zhi Hong, Brian A. Johns, Kirsten M. Kahler, Cecilia Koble, Anna Leivers, Martin R. Leivers, Amanda Mathis, Andrew J. Peat, Jeffrey J. Pouliot, Christopher D. Roberts, Vicente Samano, Rachel M. Schmidt, Gary K. Smith, Andrew Spaltenstein, Eugene L. Stewart, Pia Thommes, Elizabeth M. Turner, Christian Voitenleitner, Jill T. Walker, Greg Waitt, Jason Weatherhead, Kurt Weaver, Shawn Williams, Lois Wright, Zhiping Z. Xiong, David Haigh, and J. Brad Shotwell

Subjects
Models, Molecular, Magnetic Resonance Spectroscopy, Hepacivirus, Viral Nonstructural Proteins, Antiviral Agents, Structure-Activity Relationship, chemistry.chemical_compound, RNA polymerase, Drug Resistance, Viral, Drug Discovery, Structure–activity relationship, Replicon, Enzyme Inhibitors, NS5B, Subgenomic mRNA, Drug discovery, virus diseases, RNA-Dependent RNA Polymerase, Boronic Acids, Virology, Molecular biology, digestive system diseases, In vitro, chemistry, Molecular Medicine, Pharmacophore
Abstract

A boronic acid moiety was found to be a critical pharmacophore for enhanced in vitro potency against wild-type hepatitis C replicons and known clinical polymorphic and resistant HCV mutant replicons. The synthesis, optimization, and structure-activity relationships associated with inhibition of HCV replication in a subgenomic replication system for a series of non-nucleoside boron-containing HCV RNA-dependent RNA polymerase (NS5B) inhibitors are described. A summary of the discovery of 3 (GSK5852), a molecule which entered clinical trials in subjects infected with HCV in 2011, is included.

Published
2013

14. Structure of the Papillomavirus DNA-Tethering Complex E2:Brd4 and a Peptide that Ablates HPV Chromosomal Association

Author

Eric A. Abbate, Michael R. Botchan, and Christian Voitenleitner

Subjects
Models, Molecular, Oncogene Proteins, Fusion, Viral protein, Green Fluorescent Proteins, Molecular Sequence Data, Mitosis, Cell Cycle Proteins, Genome, Viral, Biology, Crystallography, X-Ray, Transfection, medicine.disease_cause, Chromosomes, Mice, Structure-Activity Relationship, Viral Proteins, chemistry.chemical_compound, Plasmid, medicine, Animals, Humans, Amino Acid Sequence, Molecular Biology, Peptide sequence, Metaphase, Human papillomavirus 16, Sequence Homology, Amino Acid, Nuclear Proteins, Cell Biology, Fusion protein, Molecular biology, Protein Structure, Tertiary, DNA-Binding Proteins, chemistry, DNA, Viral, Peptides, DNA, Transcription Factors
Abstract

Many DNA viruses that are latent in dividing cells are noncovalent passengers on mitotic chromosomes and require specific viral-encoded and cellular factors for this activity. The chromosomal protein Brd4 is implicated in the hitchhiking of bovine papillomavirus-1 (BPV-1), and the viral protein E2 binds to both plasmids and Brd4. Here, we present the X-ray crystal structure of the carboxy-terminal domain of Brd4 in complex with HPV-16 E2, and with this information have developed a Brd4-Tat fusion protein that is efficiently taken up by different transformed cells harboring HPV plasmids. In cells treated with these fusion proteins for only 2 hr and arrested in metaphase, the HPV DNA, either HPV-16 or -31, is displaced from mitotic chromosomes. Mutant Brd4 peptides are deficient in ablating this association. We suggest that such peptides may lead to the development of inhibitors of latency for many, if not all, papillomaviruses.

Published
2006

15. Preclinical Characterization of GSK2336805, a Novel Inhibitor of Hepatitis C Virus Replication That Selects for Resistance in NS5A

Author

Shihyun You, Maoshang Duan, Amy Wang, Ermias Woldu, Christian Voitenleitner, Katja Remlinger, Wieslaw M. Kazmierski, Renae M. Crosby, Jill Walker, Robert Hamatake, and Jessica Vamathevan

Subjects
Pharmacology, Mutation, biology, Genotype, Hepacivirus, Hepatitis C virus, viruses, biochemical phenomena, metabolism, and nutrition, medicine.disease_cause, biology.organism_classification, Virus Replication, Virology, Molecular biology, Antiviral Agents, Infectious Diseases, Viral replication, medicine, Pharmacology (medical), Replicon, NS5A, Subgenomic mRNA
Abstract

GSK2336805 is an inhibitor of hepatitis C virus (HCV) with picomolar activity on the standard genotype 1a, 1b, and 2a subgenomic replicons and exhibits a modest serum shift. GSK2336805 was not active on 22 RNA and DNA viruses that were profiled. We have identified changes in the N-terminal region of NS5A that cause a decrease in the activity of GSK2336805. These mutations in the genotype 1b replicon showed modest shifts in compound activity (

Published
2014

16. Cell Cycle-Dependent Regulation of Human DNA Polymerase α-Primase Activity by Phosphorylation

Author

Pao-Chi Liao, Christian Voitenleitner, Christoph Rehfuess, Melissa A. Hilmes, Lynda O'Rear, Douglas A. Gage, Ellen Fanning, Robert D. Ott, and Heinz-Peter Nasheuer

Subjects
DNA Replication, Phosphopeptides, Cyclin E, DNA polymerase, Recombinant Fusion Proteins, DNA polymerase II, Cyclin D, Cyclin A, DNA Primase, Protein Serine-Threonine Kinases, Peptide Mapping, Cell Line, Cyclin-dependent kinase, CDC2-CDC28 Kinases, Animals, Humans, Trypsin, Phosphorylation, Molecular Biology, S phase, Binding Sites, biology, Cell Cycle, Cyclin-Dependent Kinase 2, Cell Biology, DNA Polymerase I, DNA Dynamics and Chromosome Structure, Molecular biology, Cyclin-Dependent Kinases, biology.protein, Cyclin-dependent kinase complex
Abstract

DNA polymerase alpha-primase is known to be phosphorylated in human and yeast cells in a cell cycle-dependent manner on the p180 and p68 subunits. Here we show that phosphorylation of purified human DNA polymerase alpha-primase by purified cyclin A/cdk2 in vitro reduced its ability to initiate simian virus 40 (SV40) DNA replication in vitro, while phosphorylation by cyclin E/cdk2 stimulated its initiation activity. Tryptic phosphopeptide mapping revealed a family of p68 peptides that was modified well by cyclin A/cdk2 and poorly by cyclin E/cdk2. The p180 phosphopeptides were identical with both kinases. By mass spectrometry, the p68 peptide family was identified as residues 141 to 160. Cyclin A/cdk2- and cyclin A/cdc2-modified p68 also displayed a phosphorylation-dependent shift to slower electrophoretic mobility. Mutation of the four putative phosphorylation sites within p68 peptide residues 141 to 160 prevented its phosphorylation by cyclin A/cdk2 and the inhibition of replication activity. Phosphopeptide maps of the p68 subunit of DNA polymerase alpha-primase from human cells, synchronized and labeled in G1/S and in G2, revealed a cyclin E/cdk2-like pattern in G1/S and a cyclin A/cdk2-like pattern in G2. The slower-electrophoretic-mobility form of p68 was absent in human cells in G1/S and appeared as the cells entered G2/M. Consistent with this, the ability of DNA polymerase alpha-primase isolated from synchronized human cells to initiate SV40 replication was maximal in G1/S, decreased as the cells completed S phase, and reached a minimum in G2/M. These results suggest that the replication activity of DNA polymerase alpha-primase in human cells is regulated by phosphorylation in a cell cycle-dependent manner.

Published
1999

17. A randomized, double blind, dose escalation, first time in human study to assess the safety, tolerability, pharmacokinetics, and antiviral activity of single doses of GSK2485852 in chronically infected hepatitis C subjects

Author

David A, Wilfret, Jill, Walker, Christian, Voitenleitner, Sharon, Baptiste-Brown, Mark, Lovern, Joseph, Kim, Kimberly, Adkison, Brad, Shotwell, Amanda, Mathis, Lee, Moss, Daniel, Lee, Lou, Yu, Jianjun, Gan, and Andrew, Spaltenstein

Subjects
Adult, Male, Sulfonamides, Adolescent, Genotype, Interleukins, Hepacivirus, Hepatitis C, Chronic, Middle Aged, Viral Load, Viral Nonstructural Proteins, Antiviral Agents, Boronic Acids, United States, Food-Drug Interactions, Young Adult, Phenotype, Treatment Outcome, Double-Blind Method, Humans, RNA, Viral, Female, Protease Inhibitors, Interferons, Aged
Abstract

This first-time-in-human, randomized, double-blind, placebo-controlled, dose-escalation study assessed the safety, tolerability, pharmacokinetics, and antiviral activity of GSK2485852, a hepatitis C virus (HCV) NS5B inhibitor, in 27 chronically infected HCV genotype-1 subjects. Subjects received GSK2485852 70, 420, and 70 mg with a moderate fat/caloric meal. Safety, pharmacokinetics, antiviral activity, HCV genotype/phenotype, and interleukin 28B genotype were evaluated. A statistically significant reduction in HCV ribonucleic acid (RNA) was observed after a single dose of 420 mg GSK2485852 (-1.33 log10 IU/mL) compared with placebo (-0.09 log10 IU/mL) at 24 hours post-dose. Subjects receiving 70 mg GSK2485852 were exposed to concentrations above the protein-adjusted 90% effective concentration for a short time; none experienced a significant decline in HCV RNA (-0.47 log10 copies/mL). GSK2485852 was readily absorbed; however, the observed geometric mean maximum plasma concentration (Cmax ) and area under the curve (AUC) values were significantly lower than expected due to a higher-than-predicted-oral clearance. Co-administration with food reduced the AUC and Cmax of GSK2485852 by 40% and 70%, respectively. Two metabolites were detected in human blood with one having approximately 50% higher concentrations than those of the parent. GSK2485852 was well-tolerated and exhibited antiviral activity after a single 420 mg dose in HCV subjects.

Published
2012

18. E1 protein of bovine papillomavirus type 1 interferes with E2 protein-mediated tethering of the viral DNA to mitotic chromosomes

Author

Michael R. Botchan and Christian Voitenleitner

Subjects
DNA Replication, Transcription, Genetic, Immunology, Mitosis, Replication, Biology, Virus Replication, Microbiology, Chromosomes, Cell Line, chemistry.chemical_compound, Viral Proteins, Plasmid, Virology, Extrachromosomal DNA, Animals, Bovine papillomavirus 1, Alanine, Wild type, DNA replication, Molecular biology, Chromatin, DNA-Binding Proteins, Repressor Proteins, Viral replication, chemistry, Amino Acid Substitution, Insect Science, DNA, Viral, Mutation, DNA, Plasmids, Protein Binding
Abstract

Eukaryotic viruses can maintain latency in dividing cells as extrachromosomal plasmids. It is therefore of vital importance for viruses to ensure nuclear retention and proper segregation of their viral DNA. The bovine papillomavirus (BPV) E2 enhancer protein plays a key role in these processes by tethering the viral DNA to the host cell chromosomes. Viral genomes that harbor phosphorylation mutations in the E2 gene are transformation defective, and for these mutant genomes, neither the viral DNA nor the E2 protein is detected on mitotic chromosomes, while other key functions of E2 in transcription and replication were wild type. Moreover, secondary mutations in both the E2 and E1 proteins lead to suppression of the phosphorylation mutant phenotype and resulted in reattachment of the viral DNA and the E2 protein onto mitotic chromosomes, suggesting that E1 also plays a role in viral genome partitioning. The E1 protein was cytologically always excluded from mitotic chromatin, either as a suppressor allele or as the wild type. In the absence of other viral proteins, an E2 protein containing alanine substitutions for phosphorylation substrates in the hinge region (E2-A4) was detected as wild-type on mitotic chromosomes. However, when wild-type E1 protein levels were increased in cells expressing either the A4 mutant E2 proteins or wild-type E2, the E2-A4 protein was much more sensitive to chromosomal dislocation than was the wild-type protein. In contrast, suppressor alleles of E1 were not capable of such abrogation of E2 binding (A4 or wild-type) to chromosomes. These results suggest that wild-type E1 can be a negative regulator of the chromosomal attachment of E2.

Published
2002

19. 764 IN VITRO PROFILING OF GSK2336805, A POTENT AND SELECTIVE INHIBITOR OF HCV NS5A

Author

Jessica Vamathevan, Katrina L. Creech, Renae M. Crosby, C. Roberts, Joseph Horton, Robert Hamatake, Amy Wang, Wieslaw M. Kazmierski, L.H. Caballo, S. Van Horn, M. Duan, A. Spaltenstein, J. Bechtel, Christian Voitenleitner, and Ermias Woldu

Subjects
Hepatology, business.industry, Cancer research, Profiling (information science), Medicine, NS5A, business, In vitro
Published
2011

21. 818 PRECLINICAL CHARACTERIZATION OF GSK2485852, A NOVEL HCV POLYMERASE INHIBITOR

Author

Renae M. Crosby, Christian Voitenleitner, Jeffrey J. Pouliot, L.H. Caballo, J. Shotwell, J. Bechtel, Ermias Woldu, Amy Wang, Robert Hamatake, Katrina L. Creech, S. Van Horn, Zhi Hong, Joseph Horton, A. Spaltenstein, and Mi Xie

Subjects
education.field_of_study, Hepatology, viruses, Hepatitis C virus, Population, virus diseases, RNA-dependent RNA polymerase, biochemical phenomena, metabolism, and nutrition, Biology, medicine.disease_cause, Virology, Virus, chemistry.chemical_compound, chemistry, Genotype, medicine, Replicon, education, Gene, NS5B
Abstract

The search for direct acting antiviral (DAA) compounds that act against targets on the Hepatitis C virus or host proteins that play a crucial role in the replication of this virus is of high importance since the current standard of care does not achieve a sustained virological response (SVR) in many patients even after an extended treatment period. GSK2485852 is an inhibitor of the HCV NS5B polymerase and is highly active with EC50 values in the low nanomolar range in the genotype 1 and 2 subgenomic replicon system as well as the infectious HCV cell-culture system. In an attempt to elucidate potency of GSK2485852 beyond the standard replicon assays, we used chimeric replicon systems with NS5B genes from different genotypes as well as NS5B sequences from clinical isolates of patients infected with HCV of genotype 1a and 1b. The inhibitory activity of GSK2485852 remained unchanged on these intergenotypic and intragenotypic replicon systems. GSK2485852 furthermore displays an excellent resistance profile and shows less than a five-fold potency loss across clinically important NS5B resistance mutations like S282T, P495L, M423T, C316Y or Y448H. A diverse mutant panel tested also revealed a lack of cross resistance against known resistance mutations against other viral proteins. Data from both 454 and population sequencing showed a pattern of mutations arising in the NS5B RNA dependent RNA polymerase. GSK2485852 shows superior viral RNA reductions of up to five logs in genotype 1b replicons.

Published
2011

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