Your search keyword '"Ludmerer SW"' showing total 44 results

1. P2-Quinazolinones and Bis-Macrocycles as New Templates for Next-Generation Hepatitis C Virus NS3/4a Protease Inhibitors: Discovery of MK-2748 and MK-6325

Author

Anne Taylor, Charles J. Mcintyre, Christine Fandozzi, Carolyn McHale, Jillian DiMuzio, Steven Harper, Steven S. Carroll, Vincenzo Summa, Jeff Fritzen, Aileen Soriano, Marco Ferrara, Joseph J. Romano, David B. Olsen, Kevin Nguyen, Steven W. Ludmerer, Nigel J. Liverton, Robert Chase, Stuart Black, John W. Butcher, Kevin F. Gilbert, Qian Huang, Michael T. Rudd, Adam Gates, Paul J. Coleman, Marcello DiFilippo, Mark Stahlhut, Kimberly J. Bush, John Swestock, Nicole Trainor, Christine Burlein, Stephanie McClain, John A. McCauley, M. Katharine Holloway, Donald J. Graham, Rudd, Mt, Butcher, Jw, Nguyen, Kt, Mcintyre, Cj, Romano, Jj, Gilbert, Kf, Bush, Kj, Liverton, Nj, Holloway, Mk, Harper, S, Ferrara, M, Difilippo, M, Summa, V, Swestock, J, Fritzen, J, Carroll, S, Burlein, C, Dimuzio, Jm, Gates, A, Graham, Qian Huang, Dj, Mcclain, S, Mchale, C, Stahlhut, Mw, Black, S, Chase, R, Soriano, A, Fandozzi, C, Taylor, A, Trainor, N, Olsen, Db, Coleman, Pj, Ludmerer, Sw, and Mccauley, Ja

Subjects

Models, Molecular, Macrocyclic Compounds, medicine.medical_treatment, Mutant, Hepacivirus, Viral Nonstructural Proteins, Biology, Crystallography, X-Ray, Antiviral Agents, Biochemistry, Virus, Drug Discovery, Genotype, medicine, Hepatitis C Virus NS3/4A Protease Inhibitors, Animals, Humans, Potency, Sulfones, General Pharmacology, Toxicology and Pharmaceutics, Quinazolinones, Pharmacology, NS3, Protease, Organic Chemistry, Hepatitis C, medicine.disease, Rats, Mutation, Molecular Medicine

Abstract

With the goal of identifying inhibitors of hepatitis C virus (HCV) NS3/4a protease that are potent against a wide range of genotypes and clinically relevant mutant viruses, several subseries of macrocycles were investigated based on observations made during the discovery of MK-5172. Quinazolinone-containing macrocycles were identified as promising leads, and optimization for superior cross-genotype and mutant enzyme potency as well as rat liver and plasma concentrations following oral dosing, led to the development of MK-2748. Additional investigation of a series of bis-macrocycles containing a fused 18- and 15-membered ring system were also optimized for the same properties, leading to the discovery of MK-6325. Both compounds display the broad genotype and mutant potency necessary for clinical development as next-generation HCV NS3/4a protease inhibitors.

Published

2015

2. Multi-step parallel synthesis enabled optimization of benzofuran derivatives as pan-genotypic non-nucleoside inhibitors of HCV NS5B.

Author

Xiao D, Dai X, Liu H, He S, Shi ZC, Ludmerer SW, Li F, Nargund R, and Palani A

Subjects

Animals, Antiviral Agents chemical synthesis, Antiviral Agents pharmacokinetics, Benzofurans chemical synthesis, Benzofurans pharmacokinetics, Enzyme Inhibitors chemical synthesis, Enzyme Inhibitors pharmacokinetics, Hepacivirus enzymology, Microbial Sensitivity Tests, Molecular Structure, Rats, Wistar, Small Molecule Libraries chemical synthesis, Small Molecule Libraries pharmacokinetics, Small Molecule Libraries pharmacology, Structure-Activity Relationship, Antiviral Agents pharmacology, Benzofurans pharmacology, Enzyme Inhibitors pharmacology, Viral Nonstructural Proteins antagonists & inhibitors

Abstract

In a lead optimization effort towards NS5B NNI inhibitors, two multi-step parallel libraries were designed and successfully synthesized. Through this effort we discovered compound 9B, which achieved rigorous and delicate balance of inhibition across the common genotypes and mutants with <10 nM potency. In addition, the bicyclic compounds 9B exhibited improved FASSIF solubility over the tetracyclic compound MK-8876. This strategic approach demonstrated that, even within limited reaction scope, multi-step parallel libraries could provide access to more complex chemical space. This expedient access facilitates diverse, purpose-driven optimization of SAR and physicochemical properties., Competing Interests: Declaration of Competing Interest The authors declare that they have no known competing financial interests or personal relationships that could have appeared to influence the work reported in this paper., (Copyright © 2020 Elsevier Ltd. All rights reserved.)

Published

2020

3. Design and evaluation of novel tetracyclic benzofurans as palm site allosteric inhibitors of HCV NS5B polymerase.

Author

Liu H, Dai X, He S, Brockunier L, Marcantonio K, Ludmerer SW, Li F, Feng KI, Nargund RP, and Palani A

Subjects

Antiviral Agents chemical synthesis, Antiviral Agents chemistry, Benzofurans chemical synthesis, Benzofurans chemistry, Dose-Response Relationship, Drug, Microbial Sensitivity Tests, Molecular Structure, Structure-Activity Relationship, Viral Nonstructural Proteins metabolism, Antiviral Agents pharmacology, Benzofurans pharmacology, Drug Design, Viral Nonstructural Proteins antagonists & inhibitors

Abstract

Hepatitis C virus (HCV) NS5B polymerase is a prime target for the development of direct-acting antiviral drugs for the treatment of chronic HCV infection. Several novel and potent HCV NS5B non-nucleoside inhibitors with unique tetracyclic bezonfuran-based structures were prepared and evaluated. Similar to clinical developmental compound MK-8876, N-linked (compounds 1 and 2) and C-linked (compounds 3 and 4) tetracyclic structures maintained broad spectrum anti-replicon potency profiles and demonstrated moderate to excellent oral bioavailability and pharmacokinetic parameters across the three preclinical animal species. To better understand the importance of tetracyclic structures related to pan genotypic potency profiles especially against clinically relevant GT1a variants, the teracycles with different ring size were prepared and in vitro evaluations suggested compounds with six number ring have better overall potency profiles., (Copyright © 2019 Elsevier Ltd. All rights reserved.)

Published

2019

4. Development of a New Structural Class of Broadly Acting HCV Non-Nucleoside Inhibitors Leading to the Discovery of MK-8876.

Author

McComas CC, Palani A, Chang W, Holloway MK, Lesburg CA, Li P, Liverton N, Meinke PT, Olsen DB, Peng X, Soll RM, Ummat A, Wu J, Wu J, Zorn N, and Ludmerer SW

Subjects

Animals, Antiviral Agents pharmacokinetics, Antiviral Agents pharmacology, Benzofurans pharmacokinetics, Benzofurans pharmacology, Dogs, Hepacivirus physiology, Humans, Molecular Docking Simulation, Pan troglodytes, Rats, Viral Nonstructural Proteins metabolism, Antiviral Agents chemistry, Antiviral Agents therapeutic use, Benzofurans chemistry, Benzofurans therapeutic use, Hepacivirus drug effects, Hepatitis C drug therapy

Abstract

Studies directed at developing a broadly acting non-nucleoside inhibitor of HCV NS5B led to the discovery of a novel structural class of 5-aryl benzofurans that simultaneously interact with both the palm I and palm II binding regions. An initial candidate was potent in vitro against HCV GT1a and GT1b replicons, and induced multi-log reductions in HCV viral load when orally dosed to chronic GT1 infected chimpanzees. However, in vitro potency losses against clinically relevant GT1a variants prompted a further effort to develop compounds with sustained potency across a broader array of HCV genotypes and mutants. Ultimately, a biology and medicinal chemistry collaboration led to the discovery of the development candidate MK-8876. MK-8876 demonstrated a pan-genotypic potency profile and maintained potency against clinically relevant mutants. It demonstrated moderate bioavailability in rats and dogs, but showed low plasma clearance characteristics consistent with once-daily dosing. Herein we describe the efforts which led to the discovery of MK-8876, which advanced into Phase 1 monotherapy studies for evaluation and characterization as a component of an all-oral direct-acting drug regimen for the treatment of chronic HCV infection., (© 2017 Wiley-VCH Verlag GmbH & Co. KGaA, Weinheim.)

Published

2017

5. Vaniprevir plus peginterferon alfa-2b and ribavirin in treatment-experienced Japanese patients with hepatitis C virus genotype 1 (GT1b) infection: Phase 3 studies.

Author

Kumada H, Mochida S, Suzuki F, Chayama K, Karino Y, Nakamura K, Fujimoto G, Howe AY, Ludmerer SW, and Mobashery N

Subjects

Adult, Aged, Antiviral Agents adverse effects, Cyclopropanes, Drug Resistance, Viral genetics, Drug Therapy, Combination, Female, Hepacivirus drug effects, Hepacivirus genetics, Hepacivirus isolation & purification, Hepatitis C, Chronic virology, Humans, Indoles adverse effects, Interferon alpha-2, Interferon-alpha adverse effects, Isoindoles, Lactams, Macrocyclic, Leucine analogs & derivatives, Male, Medication Adherence statistics & numerical data, Middle Aged, Polyethylene Glycols adverse effects, Proline analogs & derivatives, RNA, Viral blood, Recombinant Proteins adverse effects, Recombinant Proteins therapeutic use, Recurrence, Ribavirin adverse effects, Sulfonamides, Viral Load drug effects, Young Adult, Antiviral Agents therapeutic use, Hepatitis C, Chronic drug therapy, Indoles therapeutic use, Interferon-alpha therapeutic use, Polyethylene Glycols therapeutic use, Ribavirin therapeutic use

Abstract

Background and Aim: Vaniprevir is a macrocyclic hepatitis C virus (HCV) non-structural (NS)3/4A protease inhibitor. The objective of these phase 3 multicenter, open-label trials was to evaluate the safety and efficacy of vaniprevir + peginterferon alfa-2b + ribavirin (PR) in Japanese patients with HCV genotype (GT)1 infection who had previously failed treatment with interferon-based regimens., Methods: Japanese patients with chronic HCV GT1 were enrolled. In PN044, patients with previous relapse or virologic breakthrough were randomized to vaniprevir (300 mg twice daily) + PR for 12 weeks followed by PR for another 12 weeks (12-week arm) or vaniprevir + PR for 24 weeks (24-week arm). In PN045, patients with previous partial/null response received vaniprevir + PR for 24 weeks. The primary endpoint was sustained virologic response at 24 weeks after completing treatment (SVR 24 )., Results: In PN044 (n = 51), SVR 24 was 92.0% and 96.2% in the 12- and 24-week arms, respectively. In PN045 (n = 42), SVR 24 was 61.9% in all patients and 55.2% in previous null responders. In both studies, vaniprevir + PR was generally safe and well tolerated; the majority of adverse events were mild/moderate and included pyrexia, decreased hemoglobin, headache, nausea, pruritus, and decreased platelet count. Polymorphisms in the HCV NS3 gene at baseline (Y56, Q80, and V170) did not impact treatment outcome. Virologic failure was principally associated with the on-treatment emergence of R155 or D168 mutations., Conclusions: Vaniprevir + PR is an effective, well-tolerated treatment for Japanese patients with HCV GT1 infection who failed previous interferon-based treatment. ClinicalTrials.gov Identifier NCT01405937 and NCT01405560 (Protocols PN044 and PN045)., (© 2016 The Authors Journal of Gastroenterology and Hepatology published by Journal of Gastroenterology and Hepatology Foundation and John Wiley & Sons Australia, Ltd.)

Published

2016

6. HCV evolutionary genetics of SVR versus virologic failure assessed from the vaniprevir phase III registration trials.

Author

Ludmerer SW, Hirano T, Black S, Howe AY, Chang W, Takase A, Nakamura K, Tanaka Y, Kumada H, Hayashi N, and Nickle D

Subjects

Amino Acid Substitution, Antiviral Agents pharmacology, Codon, Cyclopropanes, Drug Resistance, Viral, Drug Therapy, Combination, Hepacivirus classification, Humans, Indoles pharmacology, Isoindoles, Lactams, Macrocyclic, Leucine analogs & derivatives, Mutation, Phylogeny, Proline analogs & derivatives, Sequence Analysis, DNA, Sulfonamides, Treatment Failure, Treatment Outcome, Antiviral Agents therapeutic use, Evolution, Molecular, Genotype, Hepacivirus drug effects, Hepacivirus genetics, Hepatitis C drug therapy, Hepatitis C virology, Indoles therapeutic use

Abstract

Unlabelled: In the phase III registration studies conducted in Japan, Japanese HCV gt1 patients administered vaniprevir 300 mg twice daily plus pegylated interferon/ribavirin for 12 or 24 weeks achieved SVR24 rates of 83.7-84.5% among treatment-naïve patients, and 92.0-96.2% and 61.9% among breakthrough/relapsers or null-responders to prior interferon based therapy. As evidenced by direct sequencing, patients who did not achieve SVR24 principally failed due to treatment-emerging mutations at D168 or in a few cases R155. In this work, additional sequence analysis was conducted to address whether there were baseline polymorphisms associated with failure, evaluate the persistence of resistant virus among treatment failures, and assess for evidence of second site co-evolution with R155 or D168 mutations. To accomplish this, clonal sequencing (up to 40 clones per sample) was conducted on baseline, failure, and follow-up samples from all 38 patients among the vaniprevir treatment arms who met virologic failure criteria (37 gt1b, 1 gt1a, herein referred to as virologic failures) and baseline samples from 41 vaniprevir-treated SVR24 patients (all gt1b) selected among the three studies. SVR24 and virologic failure patients showed similar distributions of baseline polymorphisms previously associated with failure to one or more protease inhibitors. Furthermore, there was no evidence for baseline polymorphisms or a genetic signature across the NS3 protease domain specific to virologic failure patients, and which distinguishes them from baseline SVR24 sequences beyond a chance distribution. 24 of 32 virologic failures for whom baseline, failure, and follow-up samples were available showed reduced prevalence of the resistant virus first observed at the time of failure during the protocol-defined follow-up period of 24 weeks. Finally, pairwise analysis using either alignment or phylogenetic based methodologies provided no evidence for second site evolution with either the R155 or D168 mutations attributed to failure. This work supports and extends earlier findings based upon direct sequencing that attributed virologic failure to vaniprevir in the Phase III studies solely to the emergence of R155 or D168 mutations, with no apparent influence by other residues within the NS3 protease domain on treatment outcome. CLINICALTRIALS., Govidentifiers: NCT01370642, NCT01405937, NCT01405560., (Copyright © 2016 Elsevier B.V. All rights reserved.)

Published

2016

7. Vaniprevir plus peginterferon alfa-2b and ribavirin in treatment-naive Japanese patients with hepatitis C virus genotype 1 infection: a randomized phase III study.

Author

Hayashi N, Nakamuta M, Takehara T, Kumada H, Takase A, Howe AY, Ludmerer SW, and Mobashery N

Subjects

Adult, Aged, Antiviral Agents administration & dosage, Antiviral Agents adverse effects, Cyclopropanes, Double-Blind Method, Drug Therapy, Combination, Female, Genotype, Hepacivirus isolation & purification, Hepatitis C, Chronic virology, Humans, Interferon alpha-2, Interferon-alpha administration & dosage, Isoindoles, Japan, Lactams, Macrocyclic, Leucine analogs & derivatives, Male, Middle Aged, Polyethylene Glycols administration & dosage, Proline analogs & derivatives, Recombinant Proteins administration & dosage, Recurrence, Ribavirin administration & dosage, Sulfonamides, Treatment Outcome, Young Adult, Antiviral Agents therapeutic use, Hepacivirus genetics, Hepatitis C, Chronic drug therapy, Indoles administration & dosage

Abstract

Background: Vaniprevir is a potent macrocyclic hepatitis C virus (HCV) nonstructural protein 3/4A protease inhibitor. This phase III study evaluated the safety and efficacy of vaniprevir in combination with peginterferon alfa-2b and ribavirin (PR) for 24 weeks compared with PR alone for 48 weeks in treatment-naive Japanese patients with HCV genotype 1 infection., Methods: Treatment-naive Japanese patients with HCV genotype 1 infection were randomly assigned to receive vaniprevir (300 mg twice daily) plus PR for 12 weeks then PR alone for 12 weeks, vaniprevir (300 mg twice daily) plus PR for 24 weeks, or PR alone for 48 weeks. The primary end point was sustained virologic response 24 weeks after completion of treatment (SVR24)., Results: In total, 294 patients were randomly assigned to receive treatment. Most patients had HCV genotype 1b infection (98 %, 288 of 294 patients). SVR24 was achieved in 83.7, 84.5, and 55.1 % of the patients in the vaniprevir 12-week, vaniprevir 24-week, and control arms, respectively. The difference in SVR24 rates between each vaniprevir arm and the control arm was statistically significant (p < 0.001 for both). Relapse was commoner in the control arm (29.5 %) than in the vaniprevir arms (8.6 % and 10.5 % for the 12-week and 24-week arms, respectively). Commonly reported adverse events were generally similar across treatment arms, with the exception of an increase in the incidence of gastrointestinal adverse events such as nausea, diarrhea, and vomiting in patients receiving vaniprevir. These events were considered manageable., Conclusion: Vaniprevir is a valuable addition to the therapeutic options available to Japanese patients with HCV genotype 1 infection who are eligible for interferon-based treatment. CLINICALTRIALS., Gov Identifier: NCT01370642.

Published

2016

8. Susceptibilities of genotype 1a, 1b, and 3 hepatitis C virus variants to the NS5A inhibitor elbasvir.

Author

Liu R, Curry S, McMonagle P, Yeh WW, Ludmerer SW, Jumes PA, Marshall WL, Kong S, Ingravallo P, Black S, Pak I, DiNubile MJ, and Howe AY

Subjects

Adolescent, Adult, Female, Genotype, Hepacivirus genetics, Humans, Male, Middle Aged, Replicon genetics, Young Adult, Benzofurans pharmacology, Hepacivirus drug effects, Imidazoles pharmacology

Abstract

Elbasvir is an investigational NS5A inhibitor with in vitro activity against multiple HCV genotypes. Antiviral activity of elbasvir was measured in replicons derived from wild-type or resistant variants of genotypes 1a, 1b, and 3. The barrier to resistance was assessed by the number of resistant colonies selected by exposure to various elbasvir concentrations. In a phase 1b dose-escalating study, virologic responses were determined in 48 noncirrhotic adult men with chronic genotype 1 or 3 infections randomized to placebo or elbasvir from 5 to 50 mg (genotype 1) or 10 to 100 mg (genotype 3) once daily for 5 days. The NS5A gene was sequenced from plasma specimens obtained before, during, and after treatment. Elbasvir suppressed the emergence of resistance-associated variants (RAVs) in vitro in a dose-dependent manner. Variants selected by exposure to high elbasvir concentrations typically encoded multiple amino acid substitutions (most commonly involving loci 30, 31, and 93), conferring high-level elbasvir resistance. In the monotherapy study, patients with genotype 1b had greater reductions in HCV RNA levels than patients with genotype 1a at all elbasvir doses; responses in patients with genotype 3 were generally less pronounced than for genotype 1, particularly at lower elbasvir doses. M28T, Q30R, L31V, and Y93H in genotype 1a, L31V and Y93H in genotype 1b, and A30K, L31F, and Y93H in genotype 3 were the predominant RAVs selected by elbasvir monotherapy. Virologic findings in patients were consistent with the preclinical observations. NS5A-RAVs emerged most often at amino acid positions 28, 30, 31, and 93 in both the laboratory and clinical trial. (The MK-8742 P002 trial has been registered at ClinicalTrials.gov under identifier NCT01532973.)., (Copyright © 2015, American Society for Microbiology. All Rights Reserved.)

Published

2015

9. P2-quinazolinones and bis-macrocycles as new templates for next-generation hepatitis C virus NS3/4a protease inhibitors: discovery of MK-2748 and MK-6325.

Author

Rudd MT, Butcher JW, Nguyen KT, McIntyre CJ, Romano JJ, Gilbert KF, Bush KJ, Liverton NJ, Holloway MK, Harper S, Ferrara M, DiFilippo M, Summa V, Swestock J, Fritzen J, Carroll SS, Burlein C, DiMuzio JM, Gates A, Graham DJ, Huang Q, McClain S, McHale C, Stahlhut MW, Black S, Chase R, Soriano A, Fandozzi CM, Taylor A, Trainor N, Olsen DB, Coleman PJ, Ludmerer SW, and McCauley JA

Subjects

Animals, Antiviral Agents chemistry, Antiviral Agents pharmacokinetics, Crystallography, X-Ray, Drug Discovery, Hepacivirus drug effects, Hepacivirus genetics, Hepatitis C drug therapy, Hepatitis C virology, Humans, Macrocyclic Compounds chemistry, Macrocyclic Compounds pharmacokinetics, Models, Molecular, Mutation, Quinazolinones chemistry, Quinazolinones pharmacokinetics, Rats, Sulfones pharmacokinetics, Viral Nonstructural Proteins genetics, Antiviral Agents pharmacology, Hepacivirus enzymology, Macrocyclic Compounds pharmacology, Quinazolinones pharmacology, Sulfones pharmacology, Viral Nonstructural Proteins antagonists & inhibitors

Abstract

With the goal of identifying inhibitors of hepatitis C virus (HCV) NS3/4a protease that are potent against a wide range of genotypes and clinically relevant mutant viruses, several subseries of macrocycles were investigated based on observations made during the discovery of MK-5172. Quinazolinone-containing macrocycles were identified as promising leads, and optimization for superior cross-genotype and mutant enzyme potency as well as rat liver and plasma concentrations following oral dosing, led to the development of MK-2748. Additional investigation of a series of bis-macrocycles containing a fused 18- and 15-membered ring system were also optimized for the same properties, leading to the discovery of MK-6325. Both compounds display the broad genotype and mutant potency necessary for clinical development as next-generation HCV NS3/4a protease inhibitors., (© 2015 WILEY-VCH Verlag GmbH & Co. KGaA, Weinheim.)

Published

2015

10. Virologic resistance analysis from a phase 2 study of MK-5172 combined with pegylated interferon/ribavirin in treatment-naive patients with hepatitis C virus genotype 1 infection.

Author

Howe AY, Black S, Curry S, Ludmerer SW, Liu R, Barnard RJ, Newhard W, Hwang PM, Nickle D, Gilbert C, Caro L, DiNubile MJ, and Mobashery N

Subjects

Amides, Carbamates, Cyclopropanes, Drug Resistance, Viral, Genotype, Humans, Sulfonamides, Hepatitis C drug therapy, Interferons therapeutic use, Quinoxalines therapeutic use, Ribavirin therapeutic use

Abstract

Background: Virologic failure following treatment of hepatitis C virus (HCV) genotype 1 with direct-acting antiviral agents is often accompanied by the emergence of resistant variants. MK-5172 is an investigational once-daily protease inhibitor. We analyzed variants in treatment-naive noncirrhotic patients with virologic failure on MK-5172 (100-800 mg/day) plus pegylated interferon alfa/ribavirin (peg-IFN/RBV) during a phase 2 trial., Methods: Population and selective clonal sequencing were performed at baseline and at virologic failure in the 4 MK-5172 dosing arms. MK-5172 activity was determined using a mutant replicon assay., Results: Six of 266 (2.3%) MK-5172 recipients satisfied prespecified criteria for virologic failure, all with genotype 1a infection. Five patients with virologic failure were in the MK-5172 100-mg arm, including 4 patients with low plasma MK-5172 levels documented during triple therapy. Variants associated with >4-fold loss of potency were detected in 3 of the 4 patients with genotype 1a breakthrough while on MK-5172. The fifth patient had undetectable HCV-RNA levels at the end of triple therapy but subsequently broke through during the peg-IFN/RBV tail 16 weeks after completion of MK-5172. Three patients had D168 variants at virologic failure, including 2 with the D168A variant associated with a 95-fold loss of potency. The sole apparent relapse was actually a genotype 3a reinfection in the MK-5172 200-mg group., Conclusions: Virologic failure occurred uncommonly (6/266 [2.3%]) in MK-5172/peg-IFN/RBV recipients. The most prevalent treatment-emergent variants were detected at the D168 locus. D168A variants conferring approximately 2-log reduction in MK-5172 susceptibility emerged in 2 of the 4 evaluable patients with genotype 1a breakthrough. Clinical Trials Registration. NCT01353911., (© The Author 2014. Published by Oxford University Press on behalf of the Infectious Diseases Society of America. All rights reserved. For Permissions, please e-mail: journals.permissions@oup.com.)

Published

2014

11. Discovery of MK-8742: an HCV NS5A inhibitor with broad genotype activity.

Author

Coburn CA, Meinke PT, Chang W, Fandozzi CM, Graham DJ, Hu B, Huang Q, Kargman S, Kozlowski J, Liu R, McCauley JA, Nomeir AA, Soll RM, Vacca JP, Wang D, Wu H, Zhong B, Olsen DB, and Ludmerer SW

Subjects

Animals, Antiviral Agents chemical synthesis, Antiviral Agents pharmacokinetics, Benzofurans chemical synthesis, Benzofurans pharmacokinetics, Dogs, Drug Evaluation, Preclinical, Enzyme Inhibitors chemical synthesis, Enzyme Inhibitors pharmacokinetics, Half-Life, Hepacivirus drug effects, Hepacivirus genetics, Imidazoles chemical synthesis, Imidazoles pharmacokinetics, Indoles chemistry, Mutation, Pan troglodytes, Protein Binding, Rats, Structure-Activity Relationship, Viral Nonstructural Proteins genetics, Viral Nonstructural Proteins metabolism, Antiviral Agents chemistry, Benzofurans chemistry, Enzyme Inhibitors chemistry, Hepacivirus enzymology, Imidazoles chemistry, Viral Nonstructural Proteins antagonists & inhibitors

Abstract

The NS5A protein plays a critical role in the replication of HCV and has been the focus of numerous research efforts over the past few years. NS5A inhibitors have shown impressive in vitro potency profiles in HCV replicon assays, making them attractive components for inclusion in all oral combination regimens. Early work in the NS5A arena led to the discovery of our first clinical candidate, MK-4882 [2-((S)-pyrrolidin-2-yl)-5-(2-(4-(5-((S)-pyrrolidin-2-yl)-1H-imidazol-2-yl)phenyl)benzofuran-5-yl)-1H-imidazole]. While preclinical proof-of-concept studies in HCV-infected chimpanzees harboring chronic genotype 1 infections resulted in significant decreases in viral load after both single- and multiple-dose treatments, viral breakthrough proved to be a concern, thus necessitating the development of compounds with increased potency against a number of genotypes and NS5A resistance mutations. Modification of the MK-4882 core scaffold by introduction of a cyclic constraint afforded a series of tetracyclic inhibitors, which showed improved virologic profiles. Herein we describe the research efforts that led to the discovery of MK-8742, a tetracyclic indole-based NS5A inhibitor, which is currently in phase 2b clinical trials as part of an all-oral, interferon-free regimen for the treatment of HCV infection., (Copyright © 2013 WILEY-VCH Verlag GmbH & Co. KGaA, Weinheim.)

Published

2013

12. Development of macrocyclic inhibitors of HCV NS3/4A protease with cyclic constrained P2-P4 linkers.

Author

Rudd MT, McIntyre CJ, Romano JJ, Butcher JW, Holloway MK, Bush K, Nguyen KT, Gilbert KF, Lyle TA, Liverton NJ, Wan BL, Summa V, Harper S, Rowley M, Vacca JP, Carroll SS, Burlein C, DiMuzio JM, Gates A, Graham DJ, Huang Q, Ludmerer SW, McClain S, McHale C, Stahlhut M, Fandozzi C, Taylor A, Trainor N, Olsen DB, and McCauley JA

Subjects

Animals, Binding Sites, Carrier Proteins metabolism, Catalytic Domain, Cyclization, Genotype, Half-Life, Hepacivirus genetics, Intracellular Signaling Peptides and Proteins, Kinetics, Liver metabolism, Macrocyclic Compounds chemical synthesis, Macrocyclic Compounds pharmacokinetics, Molecular Docking Simulation, Mutation, Protease Inhibitors chemical synthesis, Protease Inhibitors pharmacokinetics, Rats, Structure-Activity Relationship, Viral Nonstructural Proteins metabolism, Carrier Proteins antagonists & inhibitors, Hepacivirus enzymology, Macrocyclic Compounds chemistry, Protease Inhibitors chemistry, Viral Nonstructural Proteins antagonists & inhibitors

Abstract

A series of macrocyclic compounds containing a cyclic constraint in the P2-P4 linker region have been discovered and shown to exhibit excellent HCV NS3/4a genotype 3a and genotype 1b R155K, A156T, A156V, and D168V mutant activity while maintaining high rat liver exposure. The effect of the constraint is most dramatic against gt 1b A156 mutants where ~20-fold improvements in potency are achieved by introduction of a variety of ring systems into the P2-P4 linker., (Copyright © 2012 Elsevier Ltd. All rights reserved.)

Published

2012

13. Development of potent macrocyclic inhibitors of genotype 3a HCV NS3/4A protease.

Author

Rudd MT, McCauley JA, Romano JJ, Butcher JW, Bush K, McIntyre CJ, Nguyen KT, Gilbert KF, Lyle TA, Holloway MK, Wan BL, Vacca JP, Summa V, Harper S, Rowley M, Carroll SS, Burlein C, DiMuzio JM, Gates A, Graham DJ, Huang Q, Ludmerer SW, McClain S, McHale C, Stahlhut M, Fandozzi C, Taylor A, Trainor N, Olsen DB, and Liverton NJ

Subjects

Animals, Carrier Proteins metabolism, Cyclization, Genotype, Half-Life, Hepacivirus genetics, Intracellular Signaling Peptides and Proteins, Kinetics, Liver metabolism, Macrocyclic Compounds chemical synthesis, Macrocyclic Compounds pharmacokinetics, Protease Inhibitors chemical synthesis, Protease Inhibitors pharmacokinetics, Quinolines chemistry, Rats, Structure-Activity Relationship, Viral Nonstructural Proteins metabolism, Carrier Proteins antagonists & inhibitors, Hepacivirus enzymology, Macrocyclic Compounds chemistry, Protease Inhibitors chemistry, Viral Nonstructural Proteins antagonists & inhibitors

Abstract

A series of macrocyclic compounds containing 2-substituted-quinoline moieties have been discovered and shown to exhibit excellent HCV NS3/4a genotype 3a and genotype 1b R155K mutant activity while maintaining the high rat liver exposure. Cyclization of the 2-substituted quinoline substituent led to a series of tricyclic P2 compounds which also display superb gt3a potency., (Copyright © 2012 Elsevier Ltd. All rights reserved.)

Published

2012

14. MK-5172, a selective inhibitor of hepatitis C virus NS3/4a protease with broad activity across genotypes and resistant variants.

Author

Summa V, Ludmerer SW, McCauley JA, Fandozzi C, Burlein C, Claudio G, Coleman PJ, Dimuzio JM, Ferrara M, Di Filippo M, Gates AT, Graham DJ, Harper S, Hazuda DJ, Huang Q, McHale C, Monteagudo E, Pucci V, Rowley M, Rudd MT, Soriano A, Stahlhut MW, Vacca JP, Olsen DB, Liverton NJ, and Carroll SS

Subjects

Amides, Animals, Antiviral Agents pharmacology, Carbamates, Cyclopropanes, Dogs, Drug Resistance, Viral, Genotype, Hepacivirus enzymology, Hepacivirus genetics, Hepatitis C, Chronic drug therapy, Hepatitis C, Chronic virology, Liver drug effects, Pan troglodytes, Quinoxalines metabolism, Rats, Sulfonamides, Viral Load drug effects, Hepacivirus drug effects, Protease Inhibitors pharmacology, Quinoxalines pharmacokinetics, Quinoxalines pharmacology, Viral Nonstructural Proteins antagonists & inhibitors

Abstract

HCV NS3/4a protease inhibitors are proven therapeutic agents against chronic hepatitis C virus infection, with boceprevir and telaprevir having recently received regulatory approval as add-on therapy to pegylated interferon/ribavirin for patients harboring genotype 1 infections. Overcoming antiviral resistance, broad genotype coverage, and a convenient dosing regimen are important attributes for future agents to be used in combinations without interferon. In this communication, we report the preclinical profile of MK-5172, a novel P2-P4 quinoxaline macrocyclic NS3/4a protease inhibitor currently in clinical development. The compound demonstrates subnanomolar activity against a broad enzyme panel encompassing major hepatitis C virus (HCV) genotypes as well as variants resistant to earlier protease inhibitors. In replicon selections, MK-5172 exerted high selective pressure, which yielded few resistant colonies. In both rat and dog, MK-5172 demonstrates good plasma and liver exposures, with 24-h liver levels suggestive of once-daily dosing. When administered to HCV-infected chimpanzees harboring chronic gt1a or gt1b infections, MK-5172 suppressed viral load between 4 to 5 logs at a dose of 1 mg/kg of body weight twice daily (b.i.d.) for 7 days. Based on its preclinical profile, MK-5172 is anticipated to be broadly active against multiple HCV genotypes and clinically important resistance variants and highly suited for incorporation into newer all-oral regimens.

Published

2012

15. Discovery of MK-5172, a Macrocyclic Hepatitis C Virus NS3/4a Protease Inhibitor.

Author

Harper S, McCauley JA, Rudd MT, Ferrara M, DiFilippo M, Crescenzi B, Koch U, Petrocchi A, Holloway MK, Butcher JW, Romano JJ, Bush KJ, Gilbert KF, McIntyre CJ, Nguyen KT, Nizi E, Carroll SS, Ludmerer SW, Burlein C, DiMuzio JM, Graham DJ, McHale CM, Stahlhut MW, Olsen DB, Monteagudo E, Cianetti S, Giuliano C, Pucci V, Trainor N, Fandozzi CM, Rowley M, Coleman PJ, Vacca JP, Summa V, and Liverton NJ

Abstract

A new class of HCV NS3/4a protease inhibitors containing a P2 to P4 macrocyclic constraint was designed using a molecular modeling-derived strategy. Building on the profile of previous clinical compounds and exploring the P2 and linker regions of the series allowed for optimization of broad genotype and mutant enzyme potency, cellular activity, and rat liver exposure following oral dosing. These studies led to the identification of clinical candidate 15 (MK-5172), which is active against genotype 1-3 NS3/4a and clinically relevant mutant enzymes and has good plasma exposure and excellent liver exposure in multiple species.

Published

2012

16. Human monoclonal antibody HCV1 effectively prevents and treats HCV infection in chimpanzees.

Author

Morin TJ, Broering TJ, Leav BA, Blair BM, Rowley KJ, Boucher EN, Wang Y, Cheslock PS, Knauber M, Olsen DB, Ludmerer SW, Szabo G, Finberg RW, Purcell RH, Lanford RE, Ambrosino DM, Molrine DC, and Babcock GJ

Subjects

Amino Acid Sequence, Animals, Cell Line, Disease Models, Animal, Hepatitis C immunology, Hepatitis C virology, Hepatitis C, Chronic immunology, Humans, Liver Transplantation, Mutation, Neutralization Tests, Pan troglodytes, RNA, Viral blood, Tetraspanin 28 metabolism, Viral Envelope Proteins genetics, Viral Envelope Proteins metabolism, Viral Load, Antibodies, Monoclonal therapeutic use, Hepacivirus immunology, Hepatitis C prevention & control, Hepatitis C Antibodies therapeutic use, Hepatitis C, Chronic therapy

Abstract

Hepatitis C virus (HCV) infection is a leading cause of liver transplantation and there is an urgent need to develop therapies to reduce rates of HCV infection of transplanted livers. Approved therapeutics for HCV are poorly tolerated and are of limited efficacy in this patient population. Human monoclonal antibody HCV1 recognizes a highly-conserved linear epitope of the HCV E2 envelope glycoprotein (amino acids 412-423) and neutralizes a broad range of HCV genotypes. In a chimpanzee model, a single dose of 250 mg/kg HCV1 delivered 30 minutes prior to infusion with genotype 1a H77 HCV provided complete protection from HCV infection, whereas a dose of 50 mg/kg HCV1 did not protect. In addition, an acutely-infected chimpanzee given 250 mg/kg HCV1 42 days following exposure to virus had a rapid reduction in viral load to below the limit of detection before rebounding 14 days later. The emergent virus displayed an E2 mutation (N415K/D) conferring resistance to HCV1 neutralization. Finally, three chronically HCV-infected chimpanzees were treated with a single dose of 40 mg/kg HCV1 and viral load was reduced to below the limit of detection for 21 days in one chimpanzee with rebounding virus displaying a resistance mutation (N417S). The other two chimpanzees had 0.5-1.0 log(10) reductions in viral load without evidence of viral resistance to HCV1. In vitro testing using HCV pseudovirus (HCVpp) demonstrated that the sera from the poorly-responding chimpanzees inhibited the ability of HCV1 to neutralize HCVpp. Measurement of antibody responses in the chronically-infected chimpanzees implicated endogenous antibody to E2 and interference with HCV1 neutralization although other factors may also be responsible. These data suggest that human monoclonal antibody HCV1 may be an effective therapeutic for the prevention of graft infection in HCV-infected patients undergoing liver transplantation.

Published

2012

17. Sustained viral response in a hepatitis C virus-infected chimpanzee via a combination of direct-acting antiviral agents.

Author

Olsen DB, Davies ME, Handt L, Koeplinger K, Zhang NR, Ludmerer SW, Graham D, Liverton N, MacCoss M, Hazuda D, and Carroll SS

Subjects

Animals, Antiviral Agents pharmacology, Antiviral Agents therapeutic use, Cyclopropanes, Dose-Response Relationship, Drug, Drug Administration Schedule, Drug Therapy, Combination, Hepacivirus enzymology, Hepacivirus physiology, Hepatitis C, Chronic virology, Indoles pharmacology, Indoles therapeutic use, Isoindoles, Lactams, Macrocyclic, Leucine analogs & derivatives, Proline analogs & derivatives, Protease Inhibitors administration & dosage, Protease Inhibitors pharmacology, Protease Inhibitors therapeutic use, Sulfonamides, Treatment Outcome, Tubercidin administration & dosage, Tubercidin pharmacology, Tubercidin therapeutic use, Viral Nonstructural Proteins antagonists & inhibitors, Antiviral Agents administration & dosage, Hepacivirus drug effects, Hepatitis C, Chronic drug therapy, Indoles administration & dosage, Pan troglodytes virology, Tubercidin analogs & derivatives, Viral Load drug effects

Abstract

Efforts to develop novel, interferon-sparing therapies for treatment of chronic hepatitis C (HCV) infection are contingent on the ability of combination therapies consisting of direct antiviral inhibitors to achieve a sustained virologic response. This work demonstrates a proof of concept that coadministration of the nucleoside analogue MK-0608 with the protease inhibitor MK-7009, both of which produced robust viral load declines as monotherapy, to an HCV-infected chimpanzee can achieve a cure of infection.

Published

2011

18. Discovery of MK-1220: A Macrocyclic Inhibitor of Hepatitis C Virus NS3/4A Protease with Improved Preclinical Plasma Exposure.

Author

Rudd MT, McCauley JA, Butcher JW, Romano JJ, McIntyre CJ, Nguyen KT, Gilbert KF, Bush KJ, Holloway MK, Swestock J, Wan BL, Carroll SS, DiMuzio JM, Graham DJ, Ludmerer SW, Stahlhut MW, Fandozzi CM, Trainor N, Olsen DB, Vacca JP, and Liverton NJ

Abstract

The discovery of MK-1220 is reported along with the development of a series of HCV NS3/4A protease inhibitors containing a P2 to P4 macrocyclic constraint with improved preclinical pharmacokinetics. Optimization of the P2 heterocycle substitution pattern as well as the P3 amino acid led to compounds with greatly improved plasma exposure following oral dosing in both rats and dogs while maintaining excellent enzyme potency and cellular activity. These studies led to the identification of MK-1220.

Published

2011

19. Discovery of vaniprevir (MK-7009), a macrocyclic hepatitis C virus NS3/4a protease inhibitor.

Author

McCauley JA, McIntyre CJ, Rudd MT, Nguyen KT, Romano JJ, Butcher JW, Gilbert KF, Bush KJ, Holloway MK, Swestock J, Wan BL, Carroll SS, DiMuzio JM, Graham DJ, Ludmerer SW, Mao SS, Stahlhut MW, Fandozzi CM, Trainor N, Olsen DB, Vacca JP, and Liverton NJ

Subjects

Animals, Area Under Curve, Carrier Proteins antagonists & inhibitors, Carrier Proteins metabolism, Cyclopropanes, Dogs, Drug Discovery, Drug Evaluation, Preclinical, Indoles chemistry, Indoles pharmacokinetics, Inhibitory Concentration 50, Intracellular Signaling Peptides and Proteins, Isoindoles, Lactams, Macrocyclic, Leucine analogs & derivatives, Liver metabolism, Macaca mulatta, Macrocyclic Compounds chemistry, Macrocyclic Compounds pharmacokinetics, Macrocyclic Compounds pharmacology, Metabolic Clearance Rate, Models, Chemical, Molecular Structure, Pan troglodytes, Proline analogs & derivatives, Rats, Serine Proteinase Inhibitors chemistry, Serine Proteinase Inhibitors pharmacokinetics, Structure-Activity Relationship, Sulfonamides, Viral Nonstructural Proteins metabolism, Viral Proteins antagonists & inhibitors, Viral Proteins metabolism, Hepacivirus enzymology, Indoles pharmacology, Serine Proteinase Inhibitors pharmacology, Viral Nonstructural Proteins antagonists & inhibitors

Abstract

A new class of HCV NS3/4a protease inhibitors which contain a P2 to P4 macrocyclic constraint was designed using a molecular-modeling derived strategy. Exploration of the P2 heterocyclic region, the P2 to P4 linker, and the P1 side chain of this class of compounds via a modular synthetic strategy allowed for the optimization of enzyme potency, cellular activity, and rat liver exposure following oral dosing. These studies led to the identification of clinical candidate 35b (vaniprevir, MK-7009), which is active against both the genotype 1 and genotype 2 NS3/4a protease enzymes and has good plasma exposure and excellent liver exposure in multiple species.

Published

2010

20. MK-7009, a potent and selective inhibitor of hepatitis C virus NS3/4A protease.

Author

Liverton NJ, Carroll SS, Dimuzio J, Fandozzi C, Graham DJ, Hazuda D, Holloway MK, Ludmerer SW, McCauley JA, McIntyre CJ, Olsen DB, Rudd MT, Stahlhut M, and Vacca JP

Subjects

Animals, Antiviral Agents pharmacokinetics, Area Under Curve, Cell Line, Cyclopropanes, Dogs, Genotype, Half-Life, Hepacivirus enzymology, Hepacivirus genetics, Humans, Indoles pharmacokinetics, Interferon alpha-2, Interferon-alpha pharmacology, Isoindoles, Lactams, Macrocyclic, Leucine analogs & derivatives, Macaca mulatta, Pan troglodytes, Proline analogs & derivatives, Protease Inhibitors pharmacokinetics, Rats, Recombinant Proteins, Replicon, Substrate Specificity, Sulfonamides, Viral Nonstructural Proteins genetics, Antiviral Agents pharmacology, Hepacivirus drug effects, Indoles pharmacology, Protease Inhibitors pharmacology, Viral Nonstructural Proteins antagonists & inhibitors

Abstract

The administration of hepatitis C virus (HCV) NS3/4A protease inhibitors to patients with chronic HCV infections has demonstrated that they have dramatic antiviral effects and that compounds acting via this mechanism are likely to form a key component of future anti-HCV therapy. We report here on the preclinical profile of MK-7009, an inhibitor of genotype 1a and 1b proteases at subnanomolar concentrations with modestly shifted potency against genotype 2a and 2b proteases at low nanomolar concentrations. Potent activity was also observed in a cell-based HCV replicon assay in the presence of added human serum (50%). In multiple species evaluated in preclinical studies, the MK-7009 concentrations in the liver were maintained at a significant multiple of the cell-based replicon 50% effective concentration over 12 to 24 h following the administration of moderate oral doses (5 to 10 mg per kg of body weight). MK-7009 also had excellent selectivity against both a range of human proteases and a broad panel of pharmacologically relevant ion channels, receptors, and enzymes. On the basis of this favorable profile, MK-7009 was selected for clinical development and is currently being evaluated in controlled clinical trials with both healthy volunteers and HCV-infected patients.

Published

2010

21. Structural basis for resistance of the genotype 2b hepatitis C virus NS5B polymerase to site A non-nucleoside inhibitors.

Author

Rydberg EH, Cellucci A, Bartholomew L, Mattu M, Barbato G, Ludmerer SW, Graham DJ, Altamura S, Paonessa G, De Francesco R, Migliaccio G, and Carfí A

Subjects

Amino Acid Substitution drug effects, Antiviral Agents chemistry, Binding Sites, Crystallography, X-Ray, DNA-Directed RNA Polymerases antagonists & inhibitors, DNA-Directed RNA Polymerases isolation & purification, Genotype, Hepacivirus drug effects, Hepacivirus genetics, Indoleacetic Acids chemistry, Indoleacetic Acids pharmacology, Kinetics, Models, Molecular, Mutant Proteins antagonists & inhibitors, Mutant Proteins chemistry, Protein Structure, Secondary, Replicon genetics, Structural Homology, Protein, Viral Nonstructural Proteins isolation & purification, Antiviral Agents pharmacology, DNA-Directed RNA Polymerases chemistry, Drug Resistance, Viral drug effects, Hepacivirus enzymology, Nucleosides pharmacology, Viral Nonstructural Proteins antagonists & inhibitors, Viral Nonstructural Proteins chemistry

Abstract

Hepatitis C virus (HCV) exists in six major genotypes. Compared with the 1b enzyme, genotype 2b HCV polymerase exhibits a more than 100-fold reduction in sensitivity to the indole-N-acetamide class of non-nucleoside inhibitors. These compounds have been shown to bind in a pocket occupied by helix A of the mobile Lambda1 loop in the apoenzyme. The three-dimensional structure of the HCV polymerase from genotype 2b was determined to 1.9-A resolution and compared with the genotype 1b enzyme. This structural analysis suggests that genotypic variants result in a different shape of the inhibitor binding site. Mutants of the inhibitor binding pocket were generated in a 1b enzyme and evaluated for their binding affinity and sensitivity to inhibition by indole-N-acetamides. Most of the point mutants showed little variation in activity and IC(50), with the exception of 15- and 7-fold increases in IC(50) for Leu392Ile and Val494Ala mutants (1b-->2b), respectively. Furthermore, a 1b replicon with 20-fold resistance to this class of inhibitors was selected and shown to contain the Leu392Ile mutation. Chimeric enzymes, where the 2b fingertip Lambda1 loop, pocket or both replaced the corresponding regions of the 1b enzyme, were also generated. The fingertip chimera retained 1b-like inhibitor binding affinity, whereas the other two chimeric constructs and the 2b enzyme displayed between 50- and 100-fold reduction in binding affinity. Together, these data suggest that differences in the amino acid composition and shape of the indole-N-acetamide binding pocket are responsible for the resistance of the 2b polymerase to this class of inhibitors.

Published

2009

22. A transient cell-based phenotype assay for hepatitis C NS3/4A protease: application to potency determinations of a novel macrocyclic inhibitor against diverse protease sequences isolated from plasma infected with HCV.

Author

Ludmerer SW, Graham DJ, Patel M, Gilbert K, Stahlhut M, and Olsen DB

Subjects

Genotype, Humans, Protease Inhibitors isolation & purification, Viral Nonstructural Proteins genetics, Hepacivirus genetics, Hepacivirus isolation & purification, Hepatitis C blood, Protease Inhibitors blood, Viral Nonstructural Proteins analysis

Abstract

The potential of hepatitis C virus (HCV) to develop antiviral resistance renders phenotypic analysis of viral relapse or breakthrough sequences essential to the clinical evaluation of HCV antivirals. This work describes a transient assay in which clinical NS3/4A sequences are co-expressed in Huh-7 cells with a reporter whose activity is an easily quantifiable measure of protease activity. The utility of the assay was demonstrated in potency evaluations of a novel protease inhibitor against panels of NS3/4A sequences spanning genotypes 1-3. The compound was potent against genotype 1a and 1b protease sequences with sub-nanomolar to low nanomolar EC(50)s, slightly diminished in potency against genotype 2b sequences, but poorly active against genotype 3a sequences. Diverse sequences of the same HCV genotype, however, varied in response to the inhibitor as much as 30-fold, with susceptibility differences not easily attributed to specific amino acid polymorphisms. The results demonstrate the versatility of a novel phenotype assay in the evaluation of a promising new class of NS3/4A inhibitor. The results highlight further the complexity in correlating susceptibility differences with specific sequence polymorphisms, and underscore the value in direct phenotyping of clinical sequences for compound sensitivity. The assay will be useful for monitoring changes in susceptibility due to emergence of resistant virus during clinical studies of protease inhibitors.

Published

2008

23. A genotype 2b NS5B polymerase with novel substitutions supports replication of a chimeric HCV 1b:2b replicon containing a genotype 1b NS3-5A background.

Author

Graham DJ, Stahlhut M, Flores O, Olsen DB, Hazuda DJ, Lafemina RL, and Ludmerer SW

Subjects

Adenosine analogs & derivatives, Adenosine pharmacology, Cell Line, Hepacivirus physiology, Humans, Models, Molecular, RNA-Dependent RNA Polymerase antagonists & inhibitors, RNA-Dependent RNA Polymerase chemistry, Ribonucleoside Diphosphate Reductase pharmacology, Species Specificity, Viral Nonstructural Proteins antagonists & inhibitors, Viral Nonstructural Proteins chemistry, Virus Replication, Hepacivirus genetics, RNA-Dependent RNA Polymerase genetics, Replicon, Viral Nonstructural Proteins genetics

Abstract

HCV diversity suggests that evaluation of HCV inhibitors for broad genotypic efficacy is warranted. The replicon system enables cell-culture compound efficacy evaluation against an active replication complex, and a functional replicon dependent upon a genotype 2b polymerase would augment existing cell-culture efficacy studies that are presently limited to genotype 1a, 1b, and 2a replicons. We made a chimeric Neo(r) 1b:2b replicon where genotype 2b NS5B was inserted into a genotype 1b NS3-5A background and transfected replicon RNA to generate Neo(r) cell lines. All cell lines contained novel substitutions within NS5B which were subsequently engineered into the parental 1b:2b replicon and shown to enhance replication to various degrees. A single NS5B M31I substitution enhanced replication to levels sufficiently robust to quantify sensitivity to HCV inhibitors in a transient replication assay. The M31I 1b:2b replicon was similarly sensitive to an active-site nucleoside inhibitor of NS5B as genotype 1b replicons, but was insensitive to two non-nucleoside inhibitors which were otherwise efficacious against the genotype 1b replicons. This work describes a novel HCV replicon sustained by a genotype 2b polymerase that is sufficiently robust for quantifiable analysis in a transient replication assay, and demonstrates its utility in characterizing anti-HCV compounds for cross-genotypic efficacy.

Published

2006

24. Replication fitness and NS5B drug sensitivity of diverse hepatitis C virus isolates characterized by using a transient replication assay.

Author

Ludmerer SW, Graham DJ, Boots E, Murray EM, Simcoe A, Markel EJ, Grobler JA, Flores OA, Olsen DB, Hazuda DJ, and LaFemina RL

Subjects

Animals, Drug Resistance, Viral, Enzyme Inhibitors pharmacology, Genotype, Hepatitis C virology, Humans, Models, Molecular, Molecular Conformation, Molecular Sequence Data, Pan troglodytes, Recombinant Fusion Proteins drug effects, Recombinant Fusion Proteins metabolism, Replicon, beta-Lactamases metabolism, Antiviral Agents pharmacology, Hepacivirus drug effects, Viral Nonstructural Proteins antagonists & inhibitors, Virus Replication drug effects

Abstract

The innate genetic variability characteristic of chronic hepatitis C virus (HCV) infection makes drug resistance a concern in the clinical development of HCV inhibitors. To address this, a transient replication assay was developed to evaluate the replication fitness and the drug sensitivity of NS5B sequences isolated from the sera of patients with chronic HCV infection. This novel assay directly compares replication between NS5B isolates, thus bypassing the potential sequence and metabolic differences which may arise with independent replicon cell lines. Patient-derived NS5B sequences were similar to those of the established HCV genotypes, but isolates from each patient shared genetic variability specific to that patient, with additional genetic variability observed across the individual isolates. Every sample provided functional NS5B isolates which supported subgenomic replication, frequently to levels comparable to that of laboratory-optimized replicons. All isolates were equivalently sensitive to an active-site nucleoside inhibitor, but the sensitivities to a panel of nonnucleoside inhibitors which targeted three distinct sites on NS5B varied among the isolates. In con1, the original laboratory-optimized replicon, the NS5B S282T substitution confers resistance to the nucleoside inhibitor but impairs replication. This substitution was engineered into both genotype 1a and genotype 1b isolates. Replication was severely debilitated, demonstrating that no compensatory residues were encoded within these genetically diverse sequences to increase the replication fitness of the mutated replicons. This work describes a transient replicon-based assay that can support the clinical development of compounds which target NS5B and demonstrates its utility by examining several patient-derived NS5B isolates for replication fitness and differential sensitivity to NS5B inhibitors.

Published

2005

25. Characterization of resistance to non-obligate chain-terminating ribonucleoside analogs that inhibit hepatitis C virus replication in vitro.

Author

Migliaccio G, Tomassini JE, Carroll SS, Tomei L, Altamura S, Bhat B, Bartholomew L, Bosserman MR, Ceccacci A, Colwell LF, Cortese R, De Francesco R, Eldrup AB, Getty KL, Hou XS, LaFemina RL, Ludmerer SW, MacCoss M, McMasters DR, Stahlhut MW, Olsen DB, Hazuda DJ, and Flores OA

Subjects

Animals, Cell Line, Drug Resistance, Viral, Male, Molecular Structure, Rats, Rats, Sprague-Dawley, Ribonucleosides chemistry, Antiviral Agents pharmacology, Hepacivirus physiology, Ribonucleosides pharmacology, Virus Replication drug effects

Abstract

The urgent need for efficacious drugs to treat chronic hepatitis C virus (HCV) infection requires a concerted effort to develop inhibitors specific for virally encoded enzymes. We demonstrate that 2'-C-methyl ribonucleosides are efficient chain-terminating inhibitors of HCV genome replication. Characterization of drug-resistant HCV replicons defined a single S282T mutation within the active site of the viral polymerase that conferred loss of sensitivity to structurally related compounds in both replicon and isolated polymerase assays. Biochemical analyses demonstrated that resistance at the level of the enzyme results from a combination of reduced affinity of the mutant polymerase for the drug and an increased ability to extend the incorporated nucleoside analog. Importantly, the combination of these agents with interferon-alpha results in synergistic inhibition of HCV genome replication in cell culture. Furthermore, 2'-C-methyl-substituted ribonucleosides also inhibited replication of genetically related viruses such as bovine diarrhea virus, yellow fever, and West African Nile viruses. These observations, together with the finding that 2'-C-methyl-guanosine in particular has a favorable pharmacological profile, suggest that this class of compounds may have broad utility in the treatment of HCV and other flavivirus infections.

Published

2003

26. Human papillomavirus type 6 virus-like particles present overlapping yet distinct conformational epitopes.

Author

Wang XM, Cook JC, Lee JC, Jansen KU, Christensen ND, Ludmerer SW, and McClements WL

Subjects

Amino Acid Sequence, Amino Acid Substitution, Antibodies, Monoclonal, Cross Reactions, Epitope Mapping, Epitopes chemistry, Epitopes genetics, Humans, Molecular Sequence Data, Mutagenesis, Site-Directed, Papillomaviridae genetics, Protein Conformation, Viral Proteins chemistry, Viral Proteins genetics, Viral Proteins immunology, Antigens, Viral chemistry, Antigens, Viral genetics, Papillomaviridae immunology

Abstract

The epitope for a human papillomavirus (HPV) type 6 conformation-dependent, neutralizing monoclonal antibody (mAb) was partially mapped using HPV L1 recombinant virus-like particles (VLPs). The mAb H6.J54 is cross-reactive with the closely related HPV types 6 and 11. By making HPV-6-like amino acid substitutions in the cottontail rabbit papillomavirus (CRPV) major capsid protein L1, we were able to transfer H6.J54 binding activity into a CRPV/HPV-6 hybrid L1 protein. Full binding activity was achieved with only nine amino acid changes and identified a region centred on the HPV-6 residues 49-54. This region has previously been shown to be a critical part of HPV-6 type-specific epitopes. Fine mapping of the region by scanning a series of alanine substitution mutations showed that in HPV-6 VLPs this type-common epitope overlaps HPV-6 type-specific epitopes.

Published

2003

27. RdlDv, a novel GABA-gated chloride channel gene from the American dog tick Dermacentor variabilis.

Author

Zheng Y, Priest B, Cully DF, and Ludmerer SW

Subjects

Amino Acid Sequence, Animals, Chloride Channels metabolism, Cloning, Molecular, Dieldrin antagonists & inhibitors, Insect Proteins biosynthesis, Insect Proteins genetics, Insecticide Resistance genetics, Ion Channel Gating, Molecular Sequence Data, Oocytes metabolism, Patch-Clamp Techniques, Picrotoxin pharmacology, Pyrazoles pharmacology, Recombinant Proteins biosynthesis, Recombinant Proteins genetics, Sequence Homology, Amino Acid, Sesterterpenes, Xenopus, gamma-Aminobutyric Acid pharmacology, Chloride Channels genetics, Dermacentor genetics, Dogs parasitology, Drosophila Proteins, Picrotoxin analogs & derivatives, Receptors, GABA-A genetics, gamma-Aminobutyric Acid metabolism

Abstract

The American dog tick Dermacentor variabilis is a major transmitter of bacterial and viral pathogens in human and animal populations, and compounds active against this species would benefit both human and animal health. Invertebrate GABA-gated chloride channels are validated targets of commonly used insecticides and acaricides. We cloned a novel member of the invertebrate GABA-gated chloride channel gene family from Dermacentor variabilis, RdlDv. The closest homologue of the predicted gene product of RdlDv is the RDL protein encoded by the GABA-gated chloride channel gene Drosophila Rdl (Resistance to Dieldrin), with which it shares 64% amino acid identity. When expressed in Xenopus oocytes, RdlDv produces GABA-activated currents blocked by the known insecticides and RDL antagonists fipronil and picrotoxinin. These results suggest that RdlDv encodes a GABA-gated chloride channel subunit, making it a potential target for compounds active against the tick D. variabilis.

Published

2003

28. Identification of a key determinant of hepatitis C virus cell culture adaptation in domain II of NS3 helicase.

Author

Grobler JA, Markel EJ, Fay JF, Graham DJ, Simcoe AL, Ludmerer SW, Murray EM, Migliaccio G, and Flores OA

Subjects

Cells, Cultured, Humans, Mutation, RNA Helicases physiology, Hepacivirus physiology, Viral Nonstructural Proteins physiology, Virus Replication genetics

Abstract

Efficient replication of hepatitis C virus (HCV) replicons in cell culture is associated with specific sequences not generally observed in vivo. These cell culture adaptive mutations dramatically increase the frequency with which replication is established in vitro. However, replicons derived from HCV isolates that have been shown to replicate in chimpanzees do not replicate in cell culture even when these adaptive mutations are introduced. To better understand this apparent paradox, we performed a gain-of-function screen to identify sequences that could confer cell culture replication competence to replicons derived from chimpanzee infectious HCV isolates. We found that residue 470 in domain II of the NS3 helicase is a critical determinant in cell culture adaptation. Substitutions in residue 470 when combined with the NS5A-S232I adaptive mutation are both necessary and sufficient to confer cell culture replication to otherwise inactive replicons, including those derived from genotype 1b HCV-BK and genotype 1a HCV-H77 isolates. The specific substitution at residue 470 required for replication is context-dependent, with R470M and P470L being optimal for the activity of HCV-BK and HCV-H77 replicons, respectively. Together these data indicate that mutations in the NS3 helicase domain II act in concert with previously identified adaptive mutations and predict that introduction of compatible residues at these positions can confer cell culture replication activity to diverse HCV isolates.

Published

2003

29. Ivermectin and nodulisporic acid receptors in Drosophila melanogaster contain both gamma-aminobutyric acid-gated Rdl and glutamate-gated GluCl alpha chloride channel subunits.

Author

Ludmerer SW, Warren VA, Williams BS, Zheng Y, Hunt DC, Ayer MB, Wallace MA, Chaudhary AG, Egan MA, Meinke PT, Dean DC, Garcia ML, Cully DF, and Smith MM

Subjects

Animals, Binding Sites, Cell Membrane metabolism, Drosophila Proteins chemistry, Drosophila melanogaster, Immune Sera metabolism, Ion Channel Gating, Precipitin Tests, Radioligand Assay, Receptors, Drug immunology, Solubility, Sulfur Radioisotopes metabolism, Chloride Channels metabolism, Drosophila Proteins physiology, Glutamic Acid physiology, Indoles metabolism, Ivermectin metabolism, Receptors, Drug metabolism, Receptors, GABA-A physiology, gamma-Aminobutyric Acid physiology

Abstract

35S-labeled derivatives of the insecticides nodulisporic acid and ivermectin were synthesized and demonstrated to bind with high affinity to a population of receptors in Drosophila head membranes that were previously shown to be associated with a glutamate-gated chloride channel. Nodulisporic acid binding was modeled as binding to a single population of receptors. Ivermectin binding was composed of at least two kinetically distinct receptor populations, only one of which was associated with nodulisporic acid binding. The binding of these two ligands was modulated by glutamate, ivermectin, and antagonists of invertebrate gamma-aminobutyric acid (GABA)ergic receptors. Because solubilized nodulisporic acid and ivermectin receptors comigrated as 230-kDa complexes by gel filtration, antisera specific for both the Drosophila glutamate-gated chloride channel subunit GluCl alpha (DmGluCl alpha) and the GABA-gated chloride channel subunit Rdl (DmRdl) proteins were generated and used to examine the possible coassembly of these two subunits within a single receptor complex. DmGluCl alpha antibodies immunoprecipitated all of the ivermectin and nodulisporic acid receptors solubilized by detergent from Drosophila head membranes. DmRdl antibodies also immunoprecipitated all solubilized nodulisporic receptors, but only approximately 70% of the ivermectin receptors. These data suggest that both DmGluCl alpha and DmRdl are components of nodulisporic acid and ivermectin receptors, and that there also exists a distinct class of ivermectin receptors that contains the DmGluCl alpha subunit but not the DmRdl subunit. This co-association of DmGluCl alpha and DmRdl represents the first biochemical and immunological evidence of coassembly of subunits from two different subclasses of ligand-gated ion channel subunits.

Published

2002

30. Identification of two novel Drosophila melanogaster histamine-gated chloride channel subunits expressed in the eye.

Author

Zheng Y, Hirschberg B, Yuan J, Wang AP, Hunt DC, Ludmerer SW, Schmatz DM, and Cully DF

Subjects

Amino Acid Sequence, Animals, Base Sequence, Chloride Channels chemistry, Chloride Channels genetics, DNA Primers, Drosophila melanogaster, Molecular Sequence Data, Phylogeny, Sequence Homology, Amino Acid, Chloride Channels physiology, Eye metabolism, Histamine physiology, Ion Channel Gating physiology

Abstract

Histamine has been shown to play a role in arthropod vision; it is the major neurotransmitter of arthropod photoreceptors. Histamine-gated chloride channels have been identified in insect optic lobes. We report the first isolation of cDNA clones encoding histamine-gated chloride channel subunits from the fruit fly Drosophila melanogaster. The encoded proteins, HisCl1 and HisCl2, share 60% amino acid identity with each other. The closest structural homologue is the human glycine alpha3 receptor, which shares 45 and 43% amino acid identity respectively. Northern hybridization analysis suggested that hisCl1 and hisCl2 mRNAs are predominantly expressed in the insect eye. Oocytes injected with in vitro transcribed RNA, encoding either HisCl1 or HisCl2, produced substantial chloride currents in response to histamine but not in response to GABA, glycine, and glutamate. The histamine sensitivity was similar to that observed in insect laminar neurons. Histamine-activated currents were not blocked by picrotoxinin, fipronil, strychnine, or the H2 antagonist cimetidine. Co-injection of both hisCl1 and hisCl2 RNAs resulted in expression of a histamine-gated chloride channel with increased sensitivity to histamine, demonstrating coassembly of the subunits. The insecticide ivermectin reversibly activated homomeric HisCl1 channels and, more potently, HisCl1 and HisCl2 heteromeric channels.

Published

2002

31. Hybrid papillomavirus L1 molecules assemble into virus-like particles that reconstitute conformational epitopes and induce neutralizing antibodies to distinct HPV types.

Author

Christensen ND, Cladel NM, Reed CA, Budgeon LR, Embers ME, Skulsky DM, McClements WL, Ludmerer SW, and Jansen KU

Subjects

Animals, Antibodies, Monoclonal immunology, Antibodies, Viral biosynthesis, Enzyme-Linked Immunosorbent Assay, Epitope Mapping, Epitopes, B-Lymphocyte chemistry, Epitopes, B-Lymphocyte genetics, Humans, Mice, Neutralization Tests, Oncogene Proteins, Viral chemistry, Oncogene Proteins, Viral genetics, Papillomaviridae genetics, Protein Conformation, Rabbits, Virion, Capsid Proteins, Epitopes, B-Lymphocyte immunology, Oncogene Proteins, Viral immunology, Papillomaviridae immunology

Abstract

Human papillomavirus (HPV) hybrid virus-like particles (VLPs) were prepared using complementary regions of the major capsid L1 proteins of HPV-11 and -16. These hybrid L1 proteins were tested for assembly into VLPs, for presentation and mapping of conformational neutralizing epitopes, and as immunogens in rabbits and mice. Two small noncontiguous hypervariable regions of HPV-16 L1, when replaced into the HPV-11 L1 backbone, produced an assembly-positive hybrid L1 which was recognized by the type-specific, conformationally dependent HPV-16 neutralizing monoclonal antibody (N-MAb) H16.V5. Several new N-MAbs that were generated following immunization of mice with wild-type HPV-16 L1 VLPs also recognized this reconstructed VLP, demonstrating that these two hypervariable regions collectively constituted an immunodominant epitope. When a set of hybrid VLPs was tested as immunogens in rabbits, antibodies to both HPV-11 and -16 wild-type L1 VLPs were obtained. One of the hybrid VLPs containing hypervariable FG and HI loops of HPV-16 L1 replaced into an HPV-11 L1 background provoked neutralizing activity against both HPV-11 and HPV-16. In addition, conformationally dependent and type-specific MAbs to both HPV-11 and HPV-16 L1 VLP were obtained from mice immunized with hybrid L1 VLPs. These data indicated that hybrid L1 proteins can be constructed that retain VLP-assembly properties, retain type-specific conformational neutralizing epitopes, can map noncontiguous regions of L1 which constitute type-specific conformational neutralizing epitopes recognized by N-MAbs, and trigger polyclonal antibodies which can neutralize antigenically unrelated HPV types., ((C)2001 Elsevier Science.)

Published

2001

32. A novel human papillomavirus type 6 neutralizing domain comprising two discrete regions of the major capsid protein L1.

Author

McClements WL, Wang XM, Ling JC, Skulsky DM, Christensen ND, Jansen KU, and Ludmerer SW

Subjects

Amino Acid Sequence, Antibodies, Monoclonal, Antibodies, Viral, Binding Sites, Capsid genetics, Consensus Sequence, Epitope Mapping, Molecular Sequence Data, Mutation, Neutralization Tests, Oncogene Proteins, Viral genetics, Papillomaviridae genetics, Viral Proteins, Capsid immunology, Capsid Proteins, Genome, Viral, Oncogene Proteins, Viral immunology, Papillomaviridae immunology

Abstract

We have mapped the binding sites on human papillomavirus (HPV) type 6 for three HPV 6-specific neutralizing monoclonal antibodies (mAbs). The critical binding residues were first identified by making HPV 11-like amino acid substitutions in the HPV 6 major capsid protein L1 and assaying the resulting virus-like particles (VLPs) for reactivity with the mAbs. To confirm the relevance of these residues for mAb binding, we demonstrated that HPV 6 type-specificity could be transferred to HPV 11 VLPs by making the appropriate HPV 6-like amino acid substitutions in the HPV 11 L1. Two binding regions were found. For one mAb, all critical residues are centered at residue 53, while for the other two mAbs, type-specific binding also requires a second site located more than 100 residues distal to the first. Both binding sites coincide with regions of L1 where the sequences of the closely related HPV 6 and 11 diverge. These regions are where the L1 sequences are the least well conserved among all HPV types and they have been implicated in type-specific binding for other HPV types. This suggests that clusters of diverged residues, surrounded by conserved L1 sequences, are presented on the surface of assembled particles and are responsible for eliciting critical humoral immune responses to the virus., (Copyright 2001 Academic Press.)

Published

2001

33. Drug-resistant Drosophila indicate glutamate-gated chloride channels are targets for the antiparasitics nodulisporic acid and ivermectin.

Author

Kane NS, Hirschberg B, Qian S, Hunt D, Thomas B, Brochu R, Ludmerer SW, Zheng Y, Smith M, Arena JP, Cohen CJ, Schmatz D, Warmke J, and Cully DF

Subjects

Animals, Base Sequence, Chloride Channels genetics, Chromosome Mapping, DNA Primers, Drosophila melanogaster, In Situ Hybridization, Indoles toxicity, Molecular Sequence Data, Phenotype, Xenopus laevis, Antiparasitic Agents pharmacology, Chloride Channels physiology, Drug Resistance, Glutamates physiology, Indoles pharmacology, Ivermectin pharmacology

Abstract

The fruit fly Drosophila melanogaster was used to examine the mode of action of the novel insecticide and acaricide nodulisporic acid. Flies resistant to nodulisporic acid were selected by stepwise increasing the dose of drug in the culture media. The resistant strain, glc(1), is at least 20-fold resistant to nodulisporic acid and 3-fold cross-resistant to the parasiticide ivermectin, and exhibited decreased brood size, decreased locomotion, and bang sensitivity. Binding assays using glc(1) head membranes showed a marked decrease in the affinity for nodulisporic acid and ivermectin. A combination of genetics and sequencing identified a proline to serine mutation (P299S) in the gene coding for the glutamate-gated chloride channel subunit DmGluClalpha. To examine the effect of this mutation on the biophysical properties of DmGluClalpha channels, it was introduced into a recombinant DmGluClalpha, and RNA encoding wild-type and mutant subunits was injected into Xenopus oocytes. Nodulisporic acid directly activated wild-type and mutant DmGluClalpha channels. However, mutant channels were approximately 10-fold less sensitive to activation by nodulisporic acid, as well as ivermectin and the endogenous ligand glutamate, providing direct evidence that nodulisporic acid and ivermectin act on DmGluClalpha channels.

Published

2000

34. HPV11 mutant virus-like particles elicit immune responses that neutralize virus and delineate a novel neutralizing domain.

Author

Ludmerer SW, McClements WL, Wang XM, Ling JC, Jansen KU, and Christensen ND

Subjects

Animals, Antibodies, Monoclonal, Antibodies, Viral, Antigens, Viral genetics, Base Sequence, Binding Sites genetics, Cell Line, DNA Primers genetics, Epitope Mapping, Humans, Immunization, Mice, Mutation, Neutralization Tests, Papillomaviridae classification, Spodoptera, Viral Vaccines immunology, Papillomaviridae genetics, Papillomaviridae immunology

Abstract

Characterization of the regions of human papillomaviruses (HPVs) that elicit neutralizing immune responses supports studies on viral infectivity and provides insight for the development and evaluation of prophylactic vaccines. HPV11 is a major etiologic agent of genital warts and a likely vaccine candidate. A conformationally dependent epitope for the binding of three neutralizing monoclonal antibodies (mAbs) has been mapped to residues G(131)T(132) of the L1 major capsid protein. The mAbs bind L1 only when it is assembled into virions or into virus-like particles (VLPs) that mimic the capsid structure. We were interested in identifying other domains of L1 that elicit neutralizing responses. To this end, we have generated a panel of mAbs against VLPs derived from HPV11 L1 harboring a G131S substitution. The new mAbs are unlike the neutralizing mAbs previously mapped to residues G(131)T(132) in that they bind both prototype and HPV11:G131S mutant VLPs. Some of the new mAbs neutralized virus in vitro. We have mapped epitopes for three of these new mAbs, as well as a neutralizing mAb generated against HPV11 virions, by measuring binding to HPV6 VLPs substituted with HPV11-like amino acids. Two regions are critical: one defined by HPV11 L1 residues 263-290 and the other by residues 346-349. mAbs H11.H3 and H11.G131S.G3 bind HPV6 VLPs with substitutions derived from the 346-349 region; in addition, H11.G131S.G3 binds HPV6 VLPs with substitutions derived only from the 263-290 region. Although H11.H3 does not bind HPV6 VLPs with substitutions derived from the 263-290 region, binding to HPV6 VLPs is enhanced when both sets of substitutions are present. mAbs H11.G131S.I1 and H11.G131S.K5 bind HPV6 VLPs with the 263-290 substitutions, but show little binding to HPV6 VLPs with the 346-349 substitutions. However, binding to HPV6 VLPs is enhanced when substitutions at both regions are present. The 346-349 region has not previously been described as eliciting a neutralizing response for any HPV type. In addition, the work demonstrates a complex binding site contributed by two distinct regions of L1., (Copyright 2000 Academic Press.)

Published

2000

35. A neutralizing epitope of human papillomavirus type 11 is principally described by a continuous set of residues which overlap a distinct linear, surface-exposed epitope.

Author

Ludmerer SW, Benincasa D, Mark GE 3rd, and Christensen ND

Subjects

Amino Acid Sequence, Animals, Antibodies, Monoclonal immunology, Binding Sites, Humans, Mice, Molecular Sequence Data, Neutralization Tests, Virion immunology, Epitopes, Papillomaviridae immunology

Abstract

A panel of monoclonal antibodies (MAbs) which neutralize human papillomavirus type 11 (HPV11) in the athymic mouse xenograph neutralization assay and bind HPV11 virus-like particles (VLPs) has been described. We recently presented evidence that the Gly131-Tyr132 residues of the major capsid protein L1 confer type 11-specific binding. However, residues distally located on the primary L1 sequence also were shown to affect binding. This poses the question whether the epitope is principally centered in the region of Gly131-Tyr132 or, alternatively, is comprised of diversely located residues which come into proximity only upon proper assembly. We analyzed the result of numerous substitutions located between Tyr123 and Val142 of the HPV11 L1 sequence. We show that substitutions at five positions result in loss of binding for one or more of these MAbs by an enzyme-linked immunosorbent assay which measures antibody binding to VLPs. We demonstrate that binding of these MAbs is redirected to HPV16 VLPs which harbor eight type 11-like substitutions within the homologous region. Three of these substitutions did not affect binding when individually substituted in HPV11 but yet were still required to transfer binding to substituted HPV16 VLPs. The results demonstrate that the epitope for this class of neutralizing MAbs, although conformational and requiring VLP assembly for presentation, principally lies along a 20-residue stretch of the L1 major capsid protein. This targets the region for evaluation of the possibility of receptor binding and suggests possibilities for the design of peptide inhibitors of virus infectivity.

Published

1997

36. Two amino acid residues confer type specificity to a neutralizing, conformationally dependent epitope on human papillomavirus type 11.

Author

Ludmerer SW, Benincasa D, and Mark GE 3rd

Subjects

Amino Acid Sequence, Animals, Antibodies, Monoclonal immunology, Antibody Specificity, Cell Line, Epitope Mapping, Humans, Molecular Sequence Data, Neutralization Tests, Protein Conformation, Sequence Homology, Amino Acid, Spodoptera, Viral Proteins, Antibodies, Viral immunology, Capsid Proteins, Epitopes, B-Lymphocyte immunology, Oncogene Proteins, Viral immunology, Papillomaviridae immunology

Abstract

Characterization of virus binding by neutralizing antibodies is important both in understanding early events in viral infectivity and in development of vaccines. Neutralizing monoclonal antibodies (MAbs) to human papillomavirus type 11 (HPV11) have been described, but mapping the binding site has been difficult because of the conformational nature of key type-specific neutralization epitopes on the L1 coat protein. We have determined those residues of the L1 protein of HPV11 which confer type specificity to the binding of HPV11-neutralizing MAbs. Binding of three HPV11-specific neutralizing MAbs could be redirected to HPV6 L1 virus-like particles in which as few as two substitutions of corresponding amino acid residues from HPV11 L1 have been made, thus demonstrating the importance of these residues to MAb binding through the transfer of a conformationally dependent epitope. In addition, a fourth neutralizing MAb could be distinguished from the other neutralizing MAbs in terms of the amino acid residues which affect binding, suggesting the possibility that it neutralizes HPV11 through a different mechanism.

Published

1996

37. Rapid, high-level transient expression of papillomavirus-like particles in insect cells.

Author

Benincasa D, Silberklang M, Mark GE 3rd, and Ludmerer SW

Subjects

Animals, Antibodies, Viral analysis, Cell Line, Cottontail rabbit papillomavirus genetics, DNA, Viral analysis, Epitopes, Oncogene Proteins, Viral biosynthesis, Rabbits, Transfection, Baculoviridae genetics, Capsid Proteins, Cottontail rabbit papillomavirus isolation & purification, Gene Expression Regulation, Viral genetics, Spodoptera virology

Abstract

Empirical scanning of natural or engineered peptide sequences for functional residues is inherently dependent upon efficient expression of large numbers of individual sequence variants to assay their relative functional potency. The insect baculovirus system has been widely used for expression of viral coat proteins, but it generally requires prior isolation and expansion of a plaque-purified recombinant viral stock to generate useful quantities of self-assembled virus-like particles. In search of a more rapid means of expression of analytical levels of the L1 coat protein of cottontail rabbit and human type 11 papilloma-viruses, we found that even brief transient cotransfection of insect cells with baculovirus plasmid transfer vectors and viral DNA yielded assembled particles that were immunologically indistinguishable from particles obtained with plaque-purified viral stocks. Within six days of plasmid/viral DNA cotransfection of Sf9 cells, at least 1-2 micrograms of assembled L1 particles/100-mm plate could be demonstrated, which proved more than sufficient to assay functionality. Transient cotransfection of insect cells should provide general utility for rapid high-level expression of sets of protein sequence variants, as well as other sequence-scanning applications such as sequence optimization in protein engineering.

Published

1996

38. Use of a novel mutagenesis strategy, optimized residue substitution, to decrease the off-rate of an anti-gp120 antibody.

Author

Lewis CM, Hollis GF, Mark GE 3rd, Tung JS, and Ludmerer SW

Subjects

Alanine genetics, Amino Acid Sequence, Base Sequence, Binding Sites, Antibody, Binding, Competitive immunology, Immunoglobulin Heavy Chains chemistry, Immunoglobulin Heavy Chains genetics, Immunoglobulin Variable Region chemistry, Immunoglobulin Variable Region genetics, Molecular Sequence Data, Antibody Affinity, HIV Antibodies biosynthesis, HIV Antibodies genetics, HIV Envelope Protein gp120 genetics, HIV Envelope Protein gp120 immunology, Mutagenesis, Insertional immunology

Abstract

We have developed a novel strategy to decrease the antibody:antigen off-rate which we call optimized residue substitution. This strategy employs alanine substitution to first identify residues non-optimal for binding, as evidenced by a decrease in off-rate upon alanine replacement. These positions are then individually randomized to all amino acids, and the best replacement for each position determined. Finally, a construct which combines all optimized substitutions is generated and evaluated. We applied this strategy to the heavy chain CDR3 of P5Q, a scFv antibody which recognizes an epitope on the V3 loop of HIV gp120. We identified two amino acid substitutions that together decrease the off-rate by nearly ten-fold. The contributions by the two substitutions were near additive, indicative of independent affects on binding. We suggest that this strategy can be generalized to strengthen protein:ligand and protein:protein interactions in other systems.

Published

1995

39. The C-terminus of the B cell activator Oct-2 functions as an activation domain in yeast.

Author

Mead J, Elliston K, Mark DF, and Ludmerer SW

Subjects

Base Sequence, DNA Probes genetics, DNA-Binding Proteins genetics, Genes, Reporter, Genetic Vectors, Host Cell Factor C1, Humans, Molecular Sequence Data, Octamer Transcription Factor-1, Octamer Transcription Factor-2, B-Lymphocytes metabolism, Saccharomyces cerevisiae genetics, Transcription Factors genetics, Transcriptional Activation

Abstract

Oct-1 and Oct-2 are human transcriptional activators that bind to the same DNA element but activate distinct sets of genes. We expressed these factors in S. cerevisiae and observed greater than 5-fold stimulation of a lacZ reporter gene only with Oct-2. Transfer of the Oct-2 C-terminal domain onto either Oct-1 (Oct1.2) or a nonactivating DNA-binding domain from GAL4 created activators capable of greater than 15 and 10-fold stimulation of activity, respectively. Thus, the C-terminus of Oct-2 is sufficient to confer activation potential to nonactive DNA-binding fragments in yeast.

Published

1994

40. Purification of glutamine tRNA synthetase from Saccharomyces cerevisiae. A monomeric aminoacyl-tRNA synthetase with a large and dispensable NH2-terminal domain.

Author

Ludmerer SW, Wright DJ, and Schimmel P

Subjects

Amino Acid Sequence, Amino Acyl-tRNA Synthetases antagonists & inhibitors, Amino Acyl-tRNA Synthetases chemistry, Animals, Antibodies, Monoclonal, Female, Mice, Mice, Inbred BALB C, Molecular Sequence Data, Peptide Fragments chemistry, Trypsin, Amino Acyl-tRNA Synthetases isolation & purification, Saccharomyces cerevisiae enzymology

Abstract

Glutamine tRNA synthetase from Saccharomyces cerevisiae has been purified to homogeneity and shown to be a monomer of 91 kDa. The size of the polypeptide agrees with that predicted from the previously reported translated DNA sequence. Mild tryptic digestion removes an amino-terminal domain and releases a fragment of 65 kDa which begins at Ser205. This tryptic fragment is similar in size and sequence to Escherichia coli glutamine tRNA synthetase and shows a modest increase from the full-length yeast enzyme in the Km values for glutamine and ATP and no difference in the kcat for aminoacylation or the Km for tRNA. Thus, the removal of the NH2-terminal domain appears to indirectly affect the ATP- and glutamine-binding sites in the nucleotide-binding fold domain to which the NH2-terminal domain is fused. A monoclonal antibody directed against the NH2-terminal domain of the full-length enzyme has little effect upon the aminoacylation activity. Therefore, over 200 amino acids of the NH2 terminus of the full-length enzyme form a domain that operationally has only a modest influence on the catalytic core of the protein. These studies reinforce the concept that eukaryotic synthetases have quasi-independent domains not found in their prokaryotic counterparts which may confer a function distinct from aminoacylation.

Published

1993

41. Identification of a glutaminyl-tRNA synthetase mutation Saccharomyces cerevisiae.

Author

Mitchell AP and Ludmerer SW

Subjects

Amino Acyl-tRNA Synthetases metabolism, Glutamates metabolism, Glutamic Acid, Glutamine metabolism, Kinetics, Mutation, Saccharomyces cerevisiae enzymology, Amino Acyl-tRNA Synthetases genetics, Genes, Genes, Fungal, Saccharomyces cerevisiae genetics

Abstract

Saccharomyces cerevisiae glutaminyl-tRNA synthetase mutants were isolated through systematic screening of tight Gln- derivatives of a leaky glutamine auxotroph. These mutations define a single nuclear gene, GLN4. The gln4-1 mutation is specific for Gln-tRNA synthetase and shows a dosage effect in heterozygous diploids. The wild-type Gln-tRNA synthetase exhibits a Km for glutamine of 25 microM; the gln4-1 mutation increases this value 20-fold. These observations strongly suggest that GLN4 encodes the Gln-tRNA synthetase.

Published

1984

42. Construction and analysis of deletions in the amino-terminal extension of glutamine tRNA synthetase of Saccharomyces cerevisiae.

Author

Ludmerer SW and Schimmel P

Subjects

Alleles, Amino Acyl-tRNA Synthetases metabolism, Base Sequence, Codon, Diploidy, Escherichia coli enzymology, Escherichia coli genetics, Genes, Fungal, Genotype, Mutation, Plasmids, Saccharomyces cerevisiae genetics, Transcription, Genetic, Amino Acyl-tRNA Synthetases genetics, Saccharomyces cerevisiae enzymology

Abstract

GLN4 of Saccharomyces cerevisiae encodes an amino-terminal extension of 224 amino acids. This is connected to a polypeptide which is colinear with and 40% identical to Escherichia coli glutamine tRNA synthetase. We examined the potential significance of the amino-terminal extension. Two single base and five multiple base frame shift deletions were constructed in this segment. Each of these mutations is associated with a lethal phenotype. This suggests that the coding sequence for the amino-terminal extension is translated. It also implies that there are no translation restarts downstream of the coding region for the amino-terminal extension which produce active enzyme. Three internal deletions of various sizes, and which preserve the correct reading frame, were constructed in the coding region of the amino-terminal extension. Cells which harbor such in-frame deletions on a multi copy plasmid are viable, even when a deletion construct is the only source of GLN4-encoded activity. Extracts of cells which have one of these deletions have reduced, but measurable, glutamine tRNA synthetase activity. We conclude that the catalytic activity resides with the segment which is homologous to the E. coli enzyme and that the amino-terminal extension itself is dispensable for aminoacylation activity. Each of the internal in-frame deletion constructions is respiration-proficient. The amino-terminal extension, therefore, is not used for an essential mitochondrial function of the GLN4 gene product. Within the accuracy of the measurements, activities of four other aminoacyl-tRNA synthetases are not affected by the presence of a GLN4 internal deletion allele as the only source of GLN4-encoded activity. This suggests that the amino-terminal extension does not stabilize a complex which includes one or more of these four enzymes and whose activity depends on proper assembly of the complex.

Published

1987

43. Gene for yeast glutamine tRNA synthetase encodes a large amino-terminal extension and provides a strong confirmation of the signature sequence for a group of the aminoacyl-tRNA synthetases.

Author

Ludmerer SW and Schimmel P

Subjects

Amino Acid Sequence, Base Sequence, Codon, DNA, Fungal genetics, DNA, Recombinant, Escherichia coli enzymology, Escherichia coli genetics, Nucleic Acid Hybridization, Saccharomyces cerevisiae genetics, Transcription, Genetic, Amino Acyl-tRNA Synthetases genetics, Saccharomyces cerevisiae enzymology

Abstract

The gene for the yeast Saccharomyces cerevisiae glutamine tRNA synthetase is shown here to encode a protein of 809 amino acids. This contrasts with the 551 amino acids of the Escherichia coli glutamine tRNA synthetase. The yeast GLN4 transcripts have 5' termini that start approximately 25 nucleotides in front of the long open reading frame. Much of the extra size of the yeast enzyme is due to a large amino-terminal extension. At codon 225, the yeast enzyme aligns with the amino terminus of the E. coli protein. From this point on, the two sequences have an average of 40% identity, with a few small gaps for alignment, until their respective carboxyl termini. At codon 254 of the yeast and codon 30 of the E. coli enzyme, however, there starts an exact 15-amino acid match between the two proteins. This match encompasses and is partially the same as a short sequence which is a signature sequence for the amino acid group of the bacterial aminoacyl-tRNA synthetases which are specific for different amino acids. This is the strongest sequence match found between any yeast cytoplasmic or mitochondrial aminoacyl-tRNA synthetase with its bacterial homologue. This region of the structure is associated with a nucleotide fold. The result provides strong validation of the signature sequence, especially for sequences where the homology relationships are less dramatic than in this example. Because the 224-amino acid extension of the yeast enzyme does not align with any part of the E. coli enzyme, we propose that it is not associated directly with the catalytic function of the enzyme. Its possible function is investigated in the accompanying paper.

Published

1987

44. Cloning of GLN4: an essential gene that encodes glutaminyl-tRNA synthetase in Saccharomyces cerevisiae.

Author

Ludmerer SW and Schimmel P

Subjects

DNA Restriction Enzymes, Genetic Complementation Test, Genotype, Mutation, Nucleic Acid Hybridization, Plasmids, Saccharomyces cerevisiae enzymology, Species Specificity, Amino Acyl-tRNA Synthetases genetics, Cloning, Molecular, Genes, Genes, Fungal, Saccharomyces cerevisiae genetics

Abstract

The structural gene for glutaminyl-tRNA synthetase has been isolated from a gene bank of Saccharomyces cerevisiae chromosomal DNA. Cloning was achieved by complementation of a recently described yeast strain that is auxotrophic for glutamine. A multicopy recombinant plasmid with a 5-kilobase-pair genomic insert conferred sixfold elevation in glutaminyl-tRNA synthetase activity and restored a Gln+ phenotype to strains that were Gln- by virtue of a mutant gln4 allele. Subfragments of the 5-kilobase insert directed integration of URA3 to GLN4. Further experiments established that GLN4 is an essential gene that is located on chromosome XV. RNA blots with a GLN4-specific probe detected a single transcript of approximately 2,900 nucleotides.

Published

1985