Your search keyword '"Lam AM"' showing total 26 results

1. Biological characterization of AB-343, a novel and potent SARS-CoV-2 M pro inhibitor with pan-coronavirus activity.

Author

McGovern-Gooch KR, Mani N, Gotchev D, Ardzinski A, Kowalski R, Sheraz M, Micolochick Steuer HM, Tercero B, Wang X, Wasserman A, Chen CY, von König K, Maskos K, Prasad A, Blaesse M, Bergmann A, Konz Makino DL, Fan KY, Kultgen SG, Lindstrom A, Nguyen D, Vega M, Wang X, Bracci N, Weiss SR, Cole AG, Lam AM, Cuconati A, and Sofia MJ

Subjects

Humans, COVID-19 virology, Chlorocebus aethiops, Vero Cells, Betacoronavirus drug effects, Protease Inhibitors pharmacology, Protease Inhibitors chemistry, Animals, Virus Replication drug effects, Viral Nonstructural Proteins antagonists & inhibitors, Viral Nonstructural Proteins metabolism, Coronavirus OC43, Human drug effects, COVID-19 Drug Treatment, Middle East Respiratory Syndrome Coronavirus drug effects, Coronavirus Infections drug therapy, Coronavirus Infections virology, SARS-CoV-2 drug effects, Antiviral Agents pharmacology, Antiviral Agents chemistry, Coronavirus 3C Proteases antagonists & inhibitors, Coronavirus 3C Proteases metabolism

Abstract

Since the SARS-CoV-2 outbreak, there have been ongoing efforts to identify antiviral molecules with broad coronavirus activity to combat COVID-19. SARS-CoV-2's main protease (M pro ) is responsible for processing the viral polypeptide into non-structural proteins essential for replication. Here, we present the biological characterization of AB-343, a covalent small-molecule inhibitor of SARS-CoV-2 M pro with potent activity in both cell-based (EC 50  = 0.018 μM) and enzymatic (K i  = 0.0028 μM) assays. AB-343 also demonstrated excellent inhibition of M pro of other human coronaviruses, including those from the alpha (229E and NL63) and beta (SARS-CoV, MERS, OC43, and HKU1) families, suggesting the compound could be active against future coronaviruses. No change in AB-343 potency was observed against M pro of SARS-CoV-2 variants of concern, including Omicron, suggesting that AB-343 could be developed as a treatment against currently circulating coronaviruses. AB-343 also remained active against several M pro variants which confer significant resistance to nirmatrelvir and ensitrelvir, which are presently the only M pro inhibitors authorized for the treatment of COVID-19, further supporting the evaluation of AB-343 as a novel and potent therapeutic for COVID-19 and other coronaviruses., Competing Interests: Declaration of competing interest The authors declare the following financial interests/personal relationships which may be considered as potential competing interests: Employees of Arbutus Biopharma may hold company stock. Other 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 © 2024 Elsevier B.V. All rights reserved.)

Published

2024

2. Structure-Activity Relationships and Discovery of ( S )-5-( tert -Butyl)-11-(difluoromethoxy)-9-methoxy-2-oxo-1,2,5,6-tetrahydropyrido[2',1':2,3]imidazo[4,5- h ]quinoline-3-carboxylic Acid (AB-161), a Novel Orally Available and Liver-Centric HBV RNA Destabilizer.

Author

Gotchev D, Chen S, Dugan B, Dorsey BD, Wang X, Sheraz M, Kowalski R, Liu F, Tang S, Chiu T, Harasym T, Graves IE, Thi EP, Mason JD, Overholt N, Dugyala R, Lam AM, Cole AG, and Sofia MJ

Subjects

Animals, Structure-Activity Relationship, Dogs, Humans, Administration, Oral, Quinolines chemistry, Quinolines pharmacology, Quinolines pharmacokinetics, RNA, Viral, Male, Rats, Drug Discovery, Hepatitis B Surface Antigens metabolism, Mice, Hepatitis B virus drug effects, Hepatitis B virus genetics, Liver metabolism, Liver drug effects, Antiviral Agents pharmacology, Antiviral Agents chemistry, Antiviral Agents pharmacokinetics, Antiviral Agents administration & dosage

Abstract

Lowering hepatitis B surface antigen (HBsAg) levels from covalently closed circular DNA (cccDNA) and the integrated genome could reduce the persistence of hepatitis B virus (HBV) infection. Since HBV replication occurs in the liver and to ameliorate the peripheral neuropathy observed with a first-generation tricyclic 4-pyridone PAPD5/7 inhibitor ( AB-452 ) having high systemic exposure, we focused on increasing the hepatocyte concentration and reducing plasma levels. Optimization of a novel series of PAPD5/7 inhibitors that decrease HBsAg levels led to the tetracyclic 2-pyridone AB-161 , which was similarly potent to AB-452 in vitro and in vivo but showed dramatically higher rodent liver-to-plasma ratios. There were no neurobehavioral effects with AB-161 in dogs up to 45 mg/kg after 60 days, unlike with AB-452 , where these were observed at lower doses by day 14. AB-161 was then advanced into 90-day GLP toxicology studies, where the improved neurotoxicity profile persisted, but reproductive issues emerged, leading to discontinuation.

Published

2024

3. Rational Design of Macrocyclic Noncovalent Inhibitors of SARS-CoV-2 M pro from a DNA-Encoded Chemical Library Screening Hit That Demonstrate Potent Inhibition against Pan-Coronavirus Homologues and Nirmatrelvir-Resistant Variants.

Author

Wang X, Gotchev D, Fan KY, Vega MM, Mani N, McGovern-Gooch K, Cuconati A, Tercero B, Wang X, Carpino P, Maskos K, Centrella PA, Schmitt A, Preuss F, Prasad A, Chen CY, Clark MA, Guilinger JP, Johnstone S, von König K, Keefe AD, Liu J, Turcotte S, Zhang Y, Konz Makino DL, Lam AM, Cole AG, and Sofia MJ

Subjects

Humans, COVID-19 Drug Treatment, Drug Resistance, Viral drug effects, Small Molecule Libraries pharmacology, Small Molecule Libraries chemistry, Structure-Activity Relationship, Macrocyclic Compounds pharmacology, Macrocyclic Compounds chemistry, Macrocyclic Compounds chemical synthesis, Molecular Docking Simulation, Protease Inhibitors pharmacology, Protease Inhibitors chemistry, Protease Inhibitors chemical synthesis, Pyrrolidines pharmacology, Pyrrolidines chemistry, Pyrrolidines chemical synthesis, Lactams, Leucine, Nitriles, Proline, SARS-CoV-2 drug effects, Antiviral Agents pharmacology, Antiviral Agents chemistry, Antiviral Agents chemical synthesis, Coronavirus 3C Proteases antagonists & inhibitors, Coronavirus 3C Proteases metabolism, Drug Design

Abstract

The recent global COVID-19 pandemic has highlighted treatments for coronavirus infection as an unmet medical need. The main protease (M pro ) has been an important target for the development of SARS-CoV-2 direct-acting antivirals. Nirmatrelvir as a covalent M pro inhibitor was the first such approved therapy. Although M pro inhibitors of various chemical classes have been reported, they are generally less active against nirmatrelvir-resistant variants and have limited pan-coronavirus potential, presenting a significant human health risk upon future outbreaks. We here present a novel approach and utilized DNA-encoded chemical library screening to identify the noncovalent M pro inhibitor 5 , which demonstrated a distinct binding mode to nirmatrelvir. A macrocyclization strategy designed to lock the active conformation resulted in lactone 12 with significantly improved antiviral activity. Further optimization led to the potent lactam 26 , which demonstrated exceptional potency against nirmatrelvir-resistant variants as well as against a panel of viral main proteases from other coronaviruses.

Published

2024

4. Preclinical and clinical antiviral characterization of AB-836, a potent capsid assembly modulator against hepatitis B virus.

Author

Lam AM, Mani N, Ardzinski A, Stever K, Cuconati A, Micolochick Steuer H, Thi EP, Graves IE, Espiritu CL, Mesaros E, Kultgen SG, Fan K, Cole AG, Harasym TO, Rijnbrand R, Brown J, Eley T, Varughese T, Gane E, Picchio G, Sims KD, and Sofia MJ

Subjects

Humans, Animals, Mice, DNA, Viral, Hep G2 Cells, Male, Female, Hepatitis B drug therapy, Hepatitis B virology, Genotype, Capsid Proteins genetics, Adult, Hepatitis B Surface Antigens, Middle Aged, Cell Line, Hepatitis B virus drug effects, Hepatitis B virus genetics, Antiviral Agents pharmacology, Virus Replication drug effects, Virus Assembly drug effects, Capsid drug effects

Abstract

HBV capsid assembly modulators (CAMs) target the core protein and inhibit pregenomic RNA encapsidation and viral replication. HBV CAMs also interfere with cccDNA formation during de novo infection, which in turn suppresses transcription and production of HBV antigens. In this report, we describe the antiviral activities of AB-836, a potent and highly selective HBV CAM. AB-836 inhibited viral replication (EC 50  = 0.010 μM) in HepDE19 cells, and cccDNA formation (EC 50  = 0.18 μM) and HBsAg production (EC 50  = 0.20 μM) in HepG2-NTCP cells during de novo infection. AB-836 showed broad genotype coverage, remained active against variants resistant to nucleos(t)ide analogs, and demonstrated improved antiviral potency against core variants resistant to other CAMs. AB-836 also mediated potent inhibition of HBV replication in a hydrodynamic injection mouse model, reducing both serum and liver HBV DNA. In a Phase 1 clinical study, 28 days of once-daily AB-836 oral dosing at 50, 100, and 200 mg resulted in mean serum HBV DNA declines of 2.57, 3.04, and 3.55 log 10 IU/mL from baseline, respectively. Neither on-treatment viral rebound nor the emergence of viral resistance was observed during the 28-day treatment period. Furthermore, HBV DNA sequence analysis of baseline samples from the Phase 1 study revealed that 51.4% of the chronic hepatitis B participants contained at least one core polymorphism within the CAM-binding pocket, suggesting that genetic variations exist at this site. While AB-836 was discontinued due to clinical safety findings, data from the preclinical and clinical studies could help inform future optimization of HBV CAMs., Competing Interests: Declaration of competing interest The authors declare the following financial interests/personal relationships which may be considered as potential competing interests: Employees of Arbutus Biopharma may hold company stock. EG reports serving on advisory boards for AbbVie, Aligos Therapeutics, Arbutus Biopharma, Gilead Sciences, Janssen, Roche, Vir and Virion Therapeutics., (Copyright © 2024 Elsevier B.V. All rights reserved.)

Published

2024

5. Control of Hepatitis B Virus with Imdusiran, a Small Interfering RNA Therapeutic.

Author

Thi EP, Ye X, Snead NM, Lee ACH, Micolochick Steuer HM, Ardzinski A, Graves IE, Espiritu C, Cuconati A, Abbott C, Jarosz A, Teng X, Paratala B, McClintock K, Harasym T, Rijnbrand R, Lam AM, and Sofia MJ

Subjects

Humans, Animals, Mice, Hepatitis B Surface Antigens genetics, Female, Disease Models, Animal, Hepatitis B virus drug effects, Hepatitis B virus genetics, Hepatitis B virus physiology, RNA, Small Interfering genetics, Antiviral Agents pharmacology, Antiviral Agents therapeutic use, Hepatitis B, Chronic drug therapy, Hepatitis B, Chronic virology, Virus Replication drug effects

Abstract

Chronic hepatitis B is a global health concern with a high risk of end-stage liver disease. Current standard-of-care agents have low cure rates, and new therapies are needed. Small interfering RNAs (siRNAs) that target viral RNAs fulfill a gap not addressed by standard-of-care agents and may contribute to a functional cure. Here, we describe the preclinical characterization of imdusiran (AB-729), a novel, pan-genotypic siRNA therapeutic that effectively reduces HBsAg, viral antigens, and viral replication in chronic hepatitis B patients and is currently in Phase 2 clinical studies. In hepatitis B virus (HBV) cell-based systems, imdusiran possessed pan-genotypic nanomolar potency and retained activity against HBV target site polymorphisms. Imdusiran was active against nucleos(t)ide analogue- and capsid assembly modulator-resistant HBV isolates, and combination with standard-of-care agents was additive. In an HBV adeno-associated virus mouse model, HBsAg was reduced up to 3.7 log 10 after a single imdusiran dose, with sustained suppression for 10 weeks. Imdusiran did not intrinsically stimulate cytokine release in healthy donor human whole blood, supportive of its mechanism of action as a direct acting RNA interference antiviral. Taken together, these data support imdusiran in combination treatment approaches toward chronic hepatitis B functional cure.

Published

2024

6. Discovery of C -Linked Nucleoside Analogues with Antiviral Activity against SARS-CoV-2.

Author

Mesaros EF, Dugan BJ, Gao M, Sheraz M, McGovern-Gooch K, Xu F, Fan KY, Nguyen D, Kultgen SG, Lindstrom A, Stever K, Tercero B, Binder RJ, Liu F, Micolochick Steuer HM, Mani N, Harasym TO, Thi EP, Cuconati A, Dorsey BD, Cole AG, Lam AM, and Sofia MJ

Subjects

Humans, Animals, Drug Discovery, Viral Nonstructural Proteins antagonists & inhibitors, Viral Nonstructural Proteins metabolism, Chlorocebus aethiops, Vero Cells, COVID-19 virology, Coronavirus RNA-Dependent RNA Polymerase, Antiviral Agents pharmacology, Antiviral Agents chemistry, SARS-CoV-2 drug effects, Nucleosides pharmacology, Nucleosides chemistry, COVID-19 Drug Treatment

Abstract

The recent COVID-19 pandemic underscored the limitations of currently available direct-acting antiviral treatments against acute respiratory RNA-viral infections and stimulated major research initiatives targeting anticoronavirus agents. Two novel nsp5 protease (MPro) inhibitors have been approved, nirmatrelvir and ensitrelvir, along with two existing nucleos(t)ide analogues repurposed as nsp12 polymerase inhibitors, remdesivir and molnupiravir, but a need still exists for therapies with improved potency and systemic exposure with oral dosing, better metabolic stability, and reduced resistance and toxicity risks. Herein, we summarize our research toward identifying nsp12 inhibitors that led to nucleoside analogues 10e and 10n , which showed favorable pan-coronavirus activity in cell-infection screens, were metabolized to active triphosphate nucleotides in cell-incubation studies, and demonstrated target (nsp12) engagement in biochemical assays.

Published

2024

7. Oxadiazepinone HBV capsid assembly modulators.

Author

Kuduk SD, Stoops B, Lam AM, Espiritu C, Vogel R, Lau V, Klumpp K, Flores OA, and Hartman GD

Subjects

Antiviral Agents chemistry, Azepines chemistry, Capsid Proteins metabolism, Dose-Response Relationship, Drug, Hepatitis B virus metabolism, Humans, Microbial Sensitivity Tests, Molecular Structure, Structure-Activity Relationship, Antiviral Agents pharmacology, Azepines pharmacology, Capsid Proteins antagonists & inhibitors, Hepatitis B virus drug effects

Abstract

The HBV core protein serves multiple essential functions in the viral life cycle that enable chronic HBV infection to persist, and as such, represents a promising drug target. Modulation of the HBV capsid assembly has shown efficacy in early clinical trials through use of small molecule capsid assembly modulators (CAMs). Herein is described the evolution and SAR of a novel pyrazolo piperidine lead series into advanced oxadiazepinone HBV CAMs., (Copyright © 2021 Elsevier Ltd. All rights reserved.)

Published

2021

8. Identification of a new class of HBV capsid assembly modulator.

Author

Kuduk SD, Stoops B, Alexander R, Lam AM, Espiritu C, Vogel R, Lau V, Klumpp K, Flores OA, and Hartman GD

Subjects

Antiviral Agents chemistry, Capsid Proteins metabolism, Dose-Response Relationship, Drug, Hepatitis B virus metabolism, Microbial Sensitivity Tests, Molecular Structure, Piperidines chemistry, Pyrazoles chemistry, Structure-Activity Relationship, Antiviral Agents pharmacology, Capsid Proteins antagonists & inhibitors, Hepatitis B virus drug effects, Piperidines pharmacology, Pyrazoles pharmacology

Abstract

The HBV core protein is a druggable target of interest due to the multiple essential functions in the HBV life cycle to enable chronic HBV infection. The core protein oligomerizes to form the viral capsid, and modulation of the HBV capsid assembly has shown efficacy in clinical trials. Herein is described the identification and hit to lead SAR of a novel series of pyrazolo piperidine HBV capsid assembly modulators., (Copyright © 2021 Elsevier Ltd. All rights reserved.)

Published

2021

9. SAR studies in the sulfonyl carboxamide class of HBV capsid assembly modulators.

Author

Kuduk SD, Lam AM, Espiritu C, Vogel R, Lau V, Klumpp K, Flores OA, and Hartman GD

Subjects

Antiviral Agents chemical synthesis, Antiviral Agents chemistry, Benzamides chemical synthesis, Benzamides chemistry, Capsid Proteins metabolism, Dose-Response Relationship, Drug, Hepatitis B virus metabolism, Humans, Microbial Sensitivity Tests, Molecular Structure, Piperidines chemical synthesis, Piperidines chemistry, Structure-Activity Relationship, Virus Assembly drug effects, Antiviral Agents pharmacology, Benzamides pharmacology, Capsid Proteins antagonists & inhibitors, Hepatitis B virus drug effects, Piperidines pharmacology

Abstract

The HBV core protein has multiple essential functions in the HBV life cycle to enable chronic HBV infection. The core protein oligomerizes to form the viral capsid, and modulation of the HBV capsid assembly process has shown clinical efficacy in early clinical trials. Herein is described the SAR exploration of NVR 3-778, the first clinical compound in the sulfonyl carboxamide class., (Copyright © 2019 Elsevier Ltd. All rights reserved.)

Published

2019

10. Preclinical Characterization of NVR 3-778, a First-in-Class Capsid Assembly Modulator against Hepatitis B Virus.

Author

Lam AM, Espiritu C, Vogel R, Ren S, Lau V, Kelly M, Kuduk SD, Hartman GD, Flores OA, and Klumpp K

Subjects

Animals, Antigens, Viral genetics, Antigens, Viral metabolism, Antiviral Agents blood, Antiviral Agents chemistry, Antiviral Agents pharmacokinetics, Benzamides blood, Benzamides chemistry, Benzamides pharmacokinetics, Capsid chemistry, Capsid metabolism, DNA, Viral genetics, DNA, Viral metabolism, Drug Evaluation, Preclinical, Female, Hep G2 Cells, Hepatitis B virology, Hepatitis B virus genetics, Hepatitis B virus metabolism, Hepatocytes drug effects, Hepatocytes pathology, Hepatocytes virology, Humans, Male, Mice, Microbial Sensitivity Tests, Piperidines blood, Piperidines chemistry, Piperidines pharmacokinetics, Primary Cell Culture, RNA, Viral genetics, RNA, Viral metabolism, Viral Core Proteins antagonists & inhibitors, Viral Core Proteins genetics, Viral Core Proteins metabolism, Virus Replication drug effects, Antiviral Agents pharmacology, Benzamides pharmacology, Capsid drug effects, DNA, Viral antagonists & inhibitors, Hepatitis B drug therapy, Hepatitis B virus drug effects, Piperidines pharmacology, RNA, Viral antagonists & inhibitors

Abstract

NVR 3-778 is the first capsid assembly modulator (CAM) that has demonstrated antiviral activity in hepatitis B virus (HBV)-infected patients. NVR 3-778 inhibited the generation of infectious HBV DNA-containing virus particles with a mean antiviral 50% effective concentration (EC 50 ) of 0.40 µM in HepG2.2.15 cells. The antiviral profile of NVR 3-778 indicates pan-genotypic antiviral activity and a lack of cross-resistance with nucleos(t)ide inhibitors of HBV replication. The combination of NVR 3-778 with nucleos(t)ide analogs in vitro resulted in additive or synergistic antiviral activity. Mutations within the hydrophobic pocket at the dimer-dimer interface of the core protein could confer resistance to NVR 3-778, which is consistent with the ability of the compound to bind to core and to induce capsid assembly. By targeting core, NVR 3-778 inhibits pregenomic RNA encapsidation, viral replication, and the production of HBV DNA- and HBV RNA-containing particles. NVR 3-778 also inhibited de novo infection and viral replication in primary human hepatocytes with EC 50 values of 0.81 µM against HBV DNA and between 3.7 and 4.8 µM against the production of HBV antigens and intracellular HBV RNA. NVR 3-778 showed favorable pharmacokinetics and safety in animal species, allowing serum levels in excess of 100 µM to be achieved in mice and, thus, enabling efficacy studies in vivo The overall preclinical profile of NVR 3-778 predicts antiviral activity in vivo and supports its further evaluation for safety, pharmacokinetics, and antiviral activity in HBV-infected patients., (Copyright © 2018 Lam et al.)

Published

2018

11. Efficacy of NVR 3-778, Alone and In Combination With Pegylated Interferon, vs Entecavir In uPA/SCID Mice With Humanized Livers and HBV Infection.

Author

Klumpp K, Shimada T, Allweiss L, Volz T, Lütgehetmann M, Hartman G, Flores OA, Lam AM, and Dandri M

Subjects

Alanine Transaminase blood, Animals, DNA, Viral genetics, Disease Models, Animal, Drug Therapy, Combination, Endoplasmic Reticulum Stress drug effects, Genotype, Guanine pharmacology, Hepatitis B diagnosis, Hepatitis B virology, Hepatitis B e Antigens blood, Hepatitis B virus genetics, Hepatitis B virus growth & development, Hepatocytes transplantation, Hepatocytes virology, Humans, Interferon Regulatory Factors genetics, Interferon Regulatory Factors metabolism, Mice, SCID, Mice, Transgenic, Phenotype, RNA, Viral genetics, Recombinant Proteins pharmacology, Serum Albumin, Human metabolism, Time Factors, Viral Load, Antiviral Agents pharmacology, Guanine analogs & derivatives, Hepatitis B drug therapy, Hepatitis B virus drug effects, Hepatocytes drug effects, Interferon-alpha pharmacology, Polyethylene Glycols pharmacology, Urokinase-Type Plasminogen Activator genetics

Abstract

Background & Aims: NVR3-778 is a capsid assembly modulator in clinical development. We determined the in vivo antiviral efficacy and effects on innate and endoplasmic reticulum (ER) stress responses of NVR3-778 alone or in combination with pegylated interferon alpha (peg-IFN) and compared with entecavir., Methods: We performed 2 studies, with a total of 61 uPA/SCID mice with humanized livers. Mice were infected with a hepatitis B virus (HBV) genotype C preparation; we waited 8 weeks for persistent infection of the human hepatocytes in livers of mice. Mice were then randomly assigned to groups (5 or 6 per group) given vehicle (control), NVR3-778, entecavir, peg-IFN, NVR3-778 + entecavir, or NVR3-778 + peg-IFN for 6 weeks. We measured levels of HB surface antigen, HB e antigen, HBV RNA, alanine aminotransferase, and human serum albumin at different time points. Livers were collected and analyzed by immunohistochemistry; levels of HBV DNA, covalently closed circular DNA, and HBV RNA, along with markers of ER stress and IFN response, were quantified., Results: Mice given NVR3-778 or entecavir alone for 6 weeks had reduced serum levels of HBV DNA compared with controls or mice given peg-IFN. The largest reduction was observed in mice given NVR3-778 + peg-IFN; in all mice in this group, the serum level of HBV DNA was below the limit of quantification. NVR3-778 and peg-IFN, but not entecavir, also reduced serum level of HBV RNA. The largest effect was obtained in the NVR3-778 + peg-IFN group, in which serum level of HBV RNA was below the limit of quantification. Levels of HB surface antigen and HB e antigen were reduced significantly in only the groups that received peg-IFN. Levels of covalently closed circular DNA did not differ significantly among groups. NVR3-778 was not associated with any significant changes in level of alanine aminotransferase, the ER stress response, or IFN-stimulated genes., Conclusions: NVR3-778 has high antiviral activity in mice with humanized livers and stable HBV infection, reducing levels of serum HBV DNA and HBV RNA. Entecavir reduced levels of serum HBV DNA, but had no effect on HBV RNA. The combination of NVR3-778 and peg-IFN prevented viral replication and HBV RNA particle production to a greater extent than each compound alone or entecavir., (Copyright © 2018 AGA Institute. Published by Elsevier Inc. All rights reserved.)

Published

2018

12. Hepatitis B Virus Capsid Assembly Modulators, but Not Nucleoside Analogs, Inhibit the Production of Extracellular Pregenomic RNA and Spliced RNA Variants.

Author

Lam AM, Ren S, Espiritu C, Kelly M, Lau V, Zheng L, Hartman GD, Flores OA, and Klumpp K

Subjects

Cell Line, DNA, Viral blood, DNA-Directed DNA Polymerase metabolism, Hepatitis B virus growth & development, Hepatocytes virology, Humans, Nucleic Acid Synthesis Inhibitors pharmacology, RNA, Viral blood, Sulfonamides pharmacology, Viral Core Proteins metabolism, Antiviral Agents pharmacology, Capsid Proteins metabolism, Hepatitis B virus drug effects, Nucleocapsid Proteins metabolism, Virus Assembly drug effects, Virus Replication drug effects

Abstract

The hepatitis B virus (HBV) core protein serves multiple essential functions in the viral life cycle, and antiviral agents that target the core protein are being developed. Capsid assembly modulators (CAMs) are compounds that target core and misdirect capsid assembly, resulting in the suppression of HBV replication and virion production. Besides HBV DNA, circulating HBV RNA has been detected in patient serum and can be associated with the treatment response. Here we studied the effect of HBV CAMs on the production of extracellular HBV RNA using infected HepaRG cells and primary human hepatocytes. Representative compounds from the sulfonamide carboxamide and heteroaryldihydropyrimidine series of CAMs were evaluated and compared to nucleos(t)ide analogs as inhibitors of the viral polymerase. The results showed that CAMs blocked extracellular HBV RNA with efficiencies similar to those with which they blocked pregenomic RNA (pgRNA) encapsidation, HBV DNA replication, and Dane particle production. Nucleos(t)ide analogs inhibited viral replication and virion production but not encapsidation or production of extracellular HBV RNA. Profiling of HBV RNA from both culture supernatants and patient serum showed that extracellular viral RNA consisted of pgRNA and spliced pgRNA variants with an internal deletion(s) but still retained the sequences at both the 5' and 3' ends. Similar variants were detected in the supernatants of infected cells with and without nucleos(t)ide analog treatment. Overall, our data demonstrate that HBV CAMs represent direct antiviral agents with a profile differentiated from that of nucleos(t)ide analogs, including the inhibition of extracellular pgRNA and spliced pgRNA., (Copyright © 2017 Lam et al.)

Published

2017

13. High-resolution crystal structure of a hepatitis B virus replication inhibitor bound to the viral core protein.

Author

Klumpp K, Lam AM, Lukacs C, Vogel R, Ren S, Espiritu C, Baydo R, Atkins K, Abendroth J, Liao G, Efimov A, Hartman G, and Flores OA

Subjects

Antiviral Agents metabolism, Antiviral Agents pharmacology, Crystallography, X-Ray, Protein Conformation, Antiviral Agents chemistry, Hepatitis B virus physiology, Viral Core Proteins metabolism, Virus Replication drug effects

Abstract

The hepatitis B virus (HBV) core protein is essential for HBV replication and an important target for antiviral drug discovery. We report the first, to our knowledge, high-resolution crystal structure of an antiviral compound bound to the HBV core protein. The compound NVR-010-001-E2 can induce assembly of the HBV core wild-type and Y132A mutant proteins and thermostabilize the proteins with a Tm increase of more than 10 °C. NVR-010-001-E2 binds at the dimer-dimer interface of the core proteins, forms a new interaction surface promoting protein-protein interaction, induces protein assembly, and increases stability. The impact of naturally occurring core protein mutations on antiviral activity correlates with NVR-010-001-E2 binding interactions determined by crystallography. The crystal structure provides understanding of a drug efficacy mechanism related to the induction and stabilization of protein-protein interactions and enables structure-guided design to improve antiviral potency and drug-like properties.

Published

2015

14. Use of 2'-spirocyclic ethers in HCV nucleoside design.

Author

Du J, Chun BK, Mosley RT, Bansal S, Bao H, Espiritu C, Lam AM, Murakami E, Niu C, Micolochick Steuer HM, Furman PA, and Sofia MJ

Subjects

Antiviral Agents chemistry, Cell Line, Cytidine chemistry, Cytidine genetics, Ethers chemistry, Magnetic Resonance Spectroscopy, Spectrometry, Mass, Electrospray Ionization, Antiviral Agents pharmacology, Cytidine pharmacology, Drug Design, Hepacivirus drug effects

Abstract

Conformationally restricted 2'-spironucleosides and their prodrugs were synthesized as potential anti-HCV agents. Although the replicon activity of the new agents containing pyrimidine bases was modest, the triphosphate of a 2'-oxetane cytidine analogue demonstrated potent intrinsic biochemical activity against the NS5B polymerase, with IC50 = 8.48 μM. Activity against NS5B bearing the S282T mutation was reduced. Phosphoramidate prodrugs of a 2'-oxetane 2-amino-6-O-methyl-purine nucleoside demonstrated potent anti-HCV activity in vitro, and the corresponding triphosphate retained similar potent activity against both wild-type and S282T HCV NS5B polymerase.

Published

2014

15. Discovery of a novel class of potent HCV NS4B inhibitors: SAR studies on piperazinone derivatives.

Author

Kakarla R, Liu J, Naduthambi D, Chang W, Mosley RT, Bao D, Steuer HM, Keilman M, Bansal S, Lam AM, Seibel W, Neilson S, Furman PA, and Sofia MJ

Subjects

Antiviral Agents chemistry, Drug Discovery, Piperazines chemistry, Structure-Activity Relationship, Antiviral Agents pharmacology, Hepacivirus drug effects, Piperazines pharmacology, Viral Nonstructural Proteins antagonists & inhibitors

Abstract

HTS screening identified compound 2a (piperazinone derivative) as a low micromolar HCV genotype 1 (GT-1) inhibitor. Resistance mapping studies suggested that this piperazinone chemotype targets the HCV nonstructural protein NS4B. Extensive SAR studies were performed around 2a and the amide function and the C-3/C-6 cis stereochemistry of the piperazinone core were essential for HCV activity. A 10-fold increase in GT-1 potency was observed when the chiral phenylcyclopropyl amide side chain of 2a was replaced with p-fluorophenylisoxazole-carbonyl moiety (67). Replacing the C-6 nonpolar hydrophobic moiety of 67 with a phenyl moiety (95) did not diminish the GT-1 potency. A heterocyclic thiophene moiety (103) and an isoxazole moiety (108) were incorporated as isosteric replacements for the C-6 phenyl moiety (95), resulting in significant improvement in GT-1b and 1a potency. However, the piperazonone class of compounds lacks GT-2 activity and, consequently, were not pursued further into development.

Published

2014

16. β-D-2'-α-F-2'-β-C-Methyl-6-O-substituted 3',5'-cyclic phosphate nucleotide prodrugs as inhibitors of hepatitis C virus replication: a structure-activity relationship study.

Author

Du J, Bao D, Chun BK, Jiang Y, Reddy PG, Zhang HR, Ross BS, Bansal S, Bao H, Espiritu C, Lam AM, Murakami E, Niu C, Micolochick Steuer HM, Furman PA, Otto MJ, and Sofia MJ

Subjects

Animals, Antiviral Agents chemical synthesis, Antiviral Agents chemistry, Dose-Response Relationship, Drug, Drug Stability, Humans, Liver drug effects, Microbial Sensitivity Tests, Models, Molecular, Molecular Structure, Nucleotides, Cyclic chemical synthesis, Nucleotides, Cyclic chemistry, Prodrugs chemical synthesis, Prodrugs chemistry, Rats, Structure-Activity Relationship, Virus Replication drug effects, Antiviral Agents pharmacology, Hepacivirus drug effects, Nucleotides, Cyclic pharmacology, Prodrugs pharmacology

Abstract

The 3',5'-cyclic phosphate prodrug 9-[β-d-2'-deoxy-2'-α-fluoro-2'-β-C-methylribofuranosyl]-2-amino-6-ethoxypurine, PSI-352938 1, has demonstrated promising anti-HCV efficacy in vitro and in human clinical trials. A structure-activity relationship study of the nucleoside 3',5'-cyclic phosphate series of β-d-2'-deoxy-2'-α-fluoro-2'-β-C-methylribofuranosyl nucleoside prodrugs was undertaken and the anti-HCV activity and in vitro safety profile were assessed. Cycloalkyl 3',5'-cyclic phosphate prodrugs were shown to be significantly more potent as inhibitors of HCV replication than branched and straight chain alkyl 3',5'-cyclic phosphate prodrugs. No cytotoxicity and mitochondrial toxicity for prodrugs 12, 13 and 19 were observed at concentrations up to 100 μm in vitro. Cycloalkyl esters of 3',5'-cyclic phosphate nucleotide prodrugs demonstrated the ability to produce high levels of active triphosphate in clone-A cells and primary human hepatocytes. Compounds 12, 13 and 19 also demonstrated the ability to effectively deliver in vivo high levels of active nucleoside phosphates to rat liver., (Copyright © 2012 Elsevier Ltd. All rights reserved.)

Published

2012

17. Metabolic activation of the anti-hepatitis C virus nucleotide prodrug PSI-352938.

Author

Niu C, Tolstykh T, Bao H, Park Y, Babusis D, Lam AM, Bansal S, Du J, Chang W, Reddy PG, Zhang HR, Woolley J, Wang LQ, Chao PB, Ray AS, Otto MJ, Sofia MJ, Furman PA, and Murakami E

Subjects

Cells, Cultured, Cytochrome P-450 CYP3A metabolism, Guanylate Kinases metabolism, Hepatocytes metabolism, Humans, Nucleoside-Diphosphate Kinase metabolism, Phosphoric Diester Hydrolases metabolism, Antiviral Agents metabolism, Cyclic P-Oxides metabolism, Hepacivirus drug effects, Nucleosides metabolism

Abstract

PSI-352938 is a novel cyclic phosphate prodrug of β-D-2'-deoxy-2'-α-fluoro-2'-β-C-methylguanosine-5'-monophosphate with potent anti-HCV activity. In order to inhibit the NS5B RNA-dependent RNA polymerase, PSI-352938 must be metabolized to the active triphosphate form, PSI-352666. During in vitro incubations with PSI-352938, significantly larger amounts of PSI-352666 were formed in primary hepatocytes than in clone A hepatitis C virus (HCV) replicon cells. Metabolism and biochemical assays were performed to define the molecular mechanism of PSI-352938 activation. The first step, removal of the isopropyl group on the 3',5'-cyclic phosphate moiety, was found to be cytochrome P450 (CYP) 3A4 dependent, with other CYP isoforms unable to catalyze the reaction. The second step, opening of the cyclic phosphate ring, was catalyzed by phosphodiesterases (PDEs) 2A1, 5A, 9A, and 11A4, all known to be expressed in the liver. The role of these enzymes in the activation of PSI-352938 was confirmed in primary human hepatocytes, where prodrug activation was reduced by inhibitors of CYP3A4 and PDEs. The third step, removal of the O(6)-ethyl group on the nucleobase, was shown to be catalyzed by adenosine deaminase-like protein 1. The resulting monophosphate was consecutively phosphorylated to the diphosphate and to the triphosphate PSI-352666 by guanylate kinase 1 and nucleoside diphosphate kinase, respectively. In addition, formation of nucleoside metabolites was observed in primary hepatocytes, and ecto-5'-nucleotidase was able to dephosphorylate the monophosphate metabolites. Since CYP3A4 is highly expressed in the liver, the CYP3A4-dependent metabolism of PSI-352938 makes it an effective liver-targeted prodrug, in part accounting for the potent antiviral activity observed clinically.

Published

2012

18. Genotype and subtype profiling of PSI-7977 as a nucleotide inhibitor of hepatitis C virus.

Author

Lam AM, Espiritu C, Bansal S, Micolochick Steuer HM, Niu C, Zennou V, Keilman M, Zhu Y, Lan S, Otto MJ, and Furman PA

Subjects

Cell Line, Genotype, Humans, Replicon drug effects, Replicon genetics, Sofosbuvir, Uridine Monophosphate pharmacology, Virus Replication drug effects, Antiviral Agents pharmacology, Hepacivirus drug effects, Hepacivirus genetics, Uridine Monophosphate analogs & derivatives

Abstract

PSI-7977, a prodrug of 2'-F-2'-C-methyluridine monophosphate, is the purified diastereoisomer of PSI-7851 and is currently being investigated in phase 3 clinical trials for the treatment of hepatitis C. In this study, we profiled the activity of PSI-7977 and its ability to select for resistance using a number of different replicon cells. Results showed that PSI-7977 was active against genotype (GT) 1a, 1b, and 2a (strain JFH-1) replicons and chimeric replicons containing GT 2a (strain J6), 2b, and 3a NS5B polymerase. Cross-resistance studies using GT 1b replicons confirmed that the S282T change conferred resistance to PSI-7977. Subsequently, we evaluated the ability of PSI-7977 to select for resistance using GT 1a, 1b, and 2a (JFH-1) replicon cells. S282T was the common mutation selected among all three genotypes, but while it conferred resistance to PSI-7977 in GT 1a and 1b, JFH-1 GT 2a S282T showed only a very modest shift in 50% effective concentration (EC(50)) for PSI-7977. Sequence analysis of the JFH-1 NS5B region indicated that additional amino acid changes were selected both prior to and after the emergence of S282T. These include T179A, M289L, I293L, M434T, and H479P. Residues 179, 289, and 293 are located within the finger and palm domains, while 434 and 479 are located on the surface of the thumb domain. Data from the JFH-1 replicon variants showed that amino acid changes within the finger and palm domains together with S282T were required to confer resistance to PSI-7977, while the mutations on the thumb domain serve to enhance the replication capacity of the S282T replicons.

Published

2012

19. Activity and the metabolic activation pathway of the potent and selective hepatitis C virus pronucleotide inhibitor PSI-353661.

Author

Furman PA, Murakami E, Niu C, Lam AM, Espiritu C, Bansal S, Bao H, Tolstykh T, Micolochick Steuer H, Keilman M, Zennou V, Bourne N, Veselenak RL, Chang W, Ross BS, Du J, Otto MJ, and Sofia MJ

Subjects

Biotransformation, Cathepsin A metabolism, Chromatography, High Pressure Liquid, Cloning, Molecular, Drug Evaluation, Preclinical, Guanosine Monophosphate antagonists & inhibitors, Guanosine Monophosphate pharmacology, Guanylate Kinases metabolism, Hep G2 Cells, Hepacivirus genetics, Hepacivirus physiology, Hepatocytes drug effects, Humans, Lactic Acid metabolism, Luciferases metabolism, Microbial Sensitivity Tests, Mitochondria drug effects, Mitochondria metabolism, Mutation, Nerve Tissue Proteins metabolism, Phenol metabolism, Phosphorylation, Prodrugs chemistry, Replicon, Viral Nonstructural Proteins antagonists & inhibitors, Antiviral Agents pharmacology, Guanosine Monophosphate analogs & derivatives, Hepacivirus drug effects, Prodrugs pharmacology, Virus Replication drug effects

Abstract

PSI-353661, a phosphoramidate prodrug of 2'-deoxy-2'-fluoro-2'-C-methylguanosine-5'-monophosphate, is a highly active inhibitor of genotype 1a, 1b, and 2a HCV RNA replication in the replicon assay and of genotype 1a and 2a infectious virus replication. PSI-353661 is active against replicons harboring the NS5B S282T or S96T/N142T amino acid alterations that confer decreased susceptibility to nucleoside/tide analogs as well as mutations that confer resistance to non-nucleoside inhibitors of NS5B. Replicon clearance studies show that PSI-353661 was able to clear cells of HCV replicon RNA and prevent a rebound in replicon RNA. PSI-353661 showed no toxicity toward bone marrow stem cells or mitochondrial toxicity. The metabolism to the active 5'-triphosphate involves hydrolysis of the carboxyl ester by cathepsin A (Cat A) and carboxylesterase 1 (CES1) followed by a putative nucleophilic attack on the phosphorus by the carboxyl group resulting in the elimination of phenol and the alaninyl phosphate metabolite, PSI-353131. Histidine triad nucleotide-binding protein 1 (Hint 1) then removes the amino acid moiety, which is followed by hydrolysis of the methoxyl group at the O(6)-position of the guanine base by adenosine deaminase-like protein 1 (ADAL1) to give 2'-deoxy-2'-fluoro-2'-C-methylguanosine-5'-monophosphate. The monophosphate is phosphorylated to the diphosphate by guanylate kinase. Nucleoside diphosphate kinase is the primary enzyme involved in phosphorylation of the diphosphate to the active triphosphate, PSI-352666. PSI-352666 is equally active against wild-type NS5B and NS5B containing the S282T amino acid alteration., (Copyright © 2011 Elsevier B.V. All rights reserved.)

Published

2011

20. Inhibition of hepatitis C virus replicon RNA synthesis by PSI-352938, a cyclic phosphate prodrug of β-D-2'-deoxy-2'-α-fluoro-2'-β-C-methylguanosine.

Author

Lam AM, Espiritu C, Murakami E, Zennou V, Bansal S, Micolochick Steuer HM, Niu C, Keilman M, Bao H, Bourne N, Veselenak RL, Reddy PG, Chang W, Du J, Nagarathnam D, Sofia MJ, Otto MJ, and Furman PA

Subjects

Deoxyguanosine pharmacology, Drug Resistance, Viral, Humans, Antiviral Agents pharmacology, Cyclic P-Oxides pharmacology, Deoxyguanosine analogs & derivatives, Hepacivirus drug effects, Nucleosides pharmacology, Prodrugs pharmacology, RNA, Viral biosynthesis, Replicon drug effects

Abstract

PSI-352938 is a novel cyclic phosphate prodrug of β-D-2'-deoxy-2'-α-fluoro-2'-β-C-methylguanosine 5'-monophosphate that has potent activity against hepatitis C virus (HCV) in vitro. The studies described here characterize the in vitro anti-HCV activity of PSI-352938, alone and in combination with other inhibitors of HCV, and the cross-resistance profile of PSI-352938. The effective concentration required to achieve 50% inhibition for PSI-352938, determined using genotype 1a-, 1b-, and 2a-derived replicons stably expressed in the Lunet cell line, were 0.20, 0.13, and 0.14 μM, respectively. The active 5'-triphosphate metabolite, PSI-352666, inhibited recombinant NS5B polymerase from genotypes 1 to 4 with comparable 50% inhibitory concentrations. In contrast, PSI-352938 did not inhibit the replication of hepatitis B virus or human immunodeficiency virus in vitro. PSI-352666 did not significantly affect the activity of human DNA and RNA polymerases. PSI-352938 and its cyclic phosphate metabolites did not affect the cyclic GMP-mediated activation of protein kinase G. Clearance studies using replicon cells demonstrated that PSI-352938 cleared cells of HCV replicon RNA and prevented replicon rebound. An additive to synergistic effect was observed when PSI-352938 was combined with other classes of HCV inhibitors, including alpha interferon, ribavirin, NS3/4A inhibitors, an NS5A inhibitor, and nucleoside/nucleotide and nonnucleoside inhibitors. Cross-resistance studies showed that PSI-352938 remained fully active against replicons containing the S282T or the S96T/N142T amino acid alteration. Replicons that contain mutations conferring resistance to various classes of nonnucleoside inhibitors also remained sensitive to inhibition by PSI-352938. PSI-352938 is currently being evaluated in a phase I clinical study in genotype 1-infected individuals.

Published

2011

21. 2'-deoxy-2'-α-fluoro-2'-β-C-methyl 3',5'-cyclic phosphate nucleotide prodrug analogs as inhibitors of HCV NS5B polymerase: discovery of PSI-352938.

Author

Reddy PG, Bao D, Chang W, Chun BK, Du J, Nagarathnam D, Rachakonda S, Ross BS, Zhang HR, Bansal S, Espiritu CL, Keilman M, Lam AM, Niu C, Steuer HM, Furman PA, Otto MJ, and Sofia MJ

Subjects

Administration, Oral, Animals, Antiviral Agents pharmacokinetics, Antiviral Agents toxicity, Cell Line, Tumor, Crystallography, X-Ray, Cyclic P-Oxides pharmacokinetics, Cyclic P-Oxides toxicity, Enzyme Inhibitors pharmacokinetics, Enzyme Inhibitors toxicity, Humans, Molecular Conformation, Nucleosides pharmacokinetics, Nucleosides toxicity, Nucleotides, Cyclic chemical synthesis, Nucleotides, Cyclic toxicity, Prodrugs pharmacokinetics, Prodrugs pharmacology, Rats, Structure-Activity Relationship, Viral Nonstructural Proteins metabolism, Antiviral Agents chemistry, Cyclic P-Oxides chemistry, Enzyme Inhibitors chemistry, Hepacivirus enzymology, Nucleosides chemistry, Nucleotides, Cyclic chemistry, Prodrugs chemistry, Viral Nonstructural Proteins antagonists & inhibitors

Abstract

A series of novel 2'-deoxy-2'-α-fluoro-2'-β-C-methyl 3',5'-cyclic phosphate nucleotide prodrug analogs were synthesized and evaluated for their in vitro anti-HCV activity and safety. These prodrugs demonstrated a 10-100-fold greater potency than the parent nucleoside in a cell-based replicon assay due to higher cellular triphosphate levels. Our structure-activity relationship (SAR) studies provided compounds that gave high levels of active triphosphate in rat liver when administered orally to rats. These studies ultimately led to the selection of the clinical development candidate 24a (PSI-352938)., (Copyright © 2010 Elsevier Ltd. All rights reserved.)

Published

2010

22. Mechanism of activation of PSI-7851 and its diastereoisomer PSI-7977.

Author

Murakami E, Tolstykh T, Bao H, Niu C, Steuer HM, Bao D, Chang W, Espiritu C, Bansal S, Lam AM, Otto MJ, Sofia MJ, and Furman PA

Subjects

Antiviral Agents pharmacology, Carboxylic Ester Hydrolases metabolism, Cathepsin A metabolism, Cell Line, Hepatocytes metabolism, Hepatocytes virology, Humans, Hydrolysis, Nucleoside-Phosphate Kinase metabolism, Prodrugs pharmacology, RNA, Viral metabolism, Sofosbuvir, Stereoisomerism, Uridine Monophosphate pharmacokinetics, Uridine Monophosphate pharmacology, Viral Nonstructural Proteins metabolism, Virus Replication physiology, Antiviral Agents pharmacokinetics, Hepacivirus physiology, Prodrugs pharmacokinetics, Uridine Monophosphate analogs & derivatives, Viral Nonstructural Proteins antagonists & inhibitors, Virus Replication drug effects

Abstract

A phosphoramidate prodrug of 2'-deoxy-2'-α-fluoro-β-C-methyluridine-5'-monophosphate, PSI-7851, demonstrates potent anti-hepatitis C virus (HCV) activity both in vitro and in vivo. PSI-7851 is a mixture of two diastereoisomers, PSI-7976 and PSI-7977, with PSI-7977 being the more active inhibitor of HCV RNA replication in the HCV replicon assay. To inhibit the HCV NS5B RNA-dependent RNA polymerase, PSI-7851 must be metabolized to the active triphosphate form. The first step, hydrolysis of the carboxyl ester by human cathepsin A (CatA) and/or carboxylesterase 1 (CES1), is a stereospecific reaction. Western blot analysis showed that CatA and CES1 are both expressed in primary human hepatocytes. However, expression of CES1 is undetectable in clone A replicon cells. Studies with inhibitors of CatA and/or CES1 indicated that CatA is primarily responsible for hydrolysis of the carboxyl ester in clone A cells, although in primary human hepatocytes, both CatA and CES1 contribute to the hydrolysis. Hydrolysis of the ester is followed by a putative nucleophilic attack on the phosphorus by the carboxyl group resulting in the spontaneous elimination of phenol and the production of an alaninyl phosphate metabolite, PSI-352707, which is common to both isomers. The removal of the amino acid moiety of PSI-352707 is catalyzed by histidine triad nucleotide-binding protein 1 (Hint1) to give the 5'-monophosphate form, PSI-7411. siRNA-mediated Hint1 knockdown studies further indicate that Hint1 is, at least in part, responsible for converting PSI-352707 to PSI-7411. PSI-7411 is then consecutively phosphorylated to the diphosphate, PSI-7410, and to the active triphosphate metabolite, PSI-7409, by UMP-CMP kinase and nucleoside diphosphate kinase, respectively.

Published

2010

23. Discovery of a β-d-2'-deoxy-2'-α-fluoro-2'-β-C-methyluridine nucleotide prodrug (PSI-7977) for the treatment of hepatitis C virus.

Author

Sofia MJ, Bao D, Chang W, Du J, Nagarathnam D, Rachakonda S, Reddy PG, Ross BS, Wang P, Zhang HR, Bansal S, Espiritu C, Keilman M, Lam AM, Steuer HM, Niu C, Otto MJ, and Furman PA

Subjects

Animals, Antiviral Agents pharmacokinetics, Antiviral Agents pharmacology, Cell Line, Crystallography, X-Ray, Dogs, Drug Resistance, Viral, Esters, Hepacivirus genetics, Hepatocytes metabolism, Humans, In Vitro Techniques, Liver metabolism, Macaca fascicularis, Mutation, Prodrugs pharmacokinetics, Prodrugs pharmacology, Rats, Replicon, Sofosbuvir, Stereoisomerism, Structure-Activity Relationship, Uridine Monophosphate chemical synthesis, Uridine Monophosphate pharmacokinetics, Uridine Monophosphate pharmacology, Viral Nonstructural Proteins genetics, Antiviral Agents chemical synthesis, Hepacivirus drug effects, Prodrugs chemical synthesis, Uridine Monophosphate analogs & derivatives, Viral Nonstructural Proteins antagonists & inhibitors

Abstract

Hepatitis C virus (HCV) is a global health problem requiring novel approaches for effective treatment of this disease. The HCV NS5B polymerase has been demonstrated to be a viable target for the development of HCV therapies. β-d-2'-Deoxy-2'-α-fluoro-2'-β-C-methyl nucleosides are selective inhibitors of the HCV NS5B polymerase and have demonstrated potent activity in the clinic. Phosphoramidate prodrugs of the 5'-phosphate derivative of the β-d-2'-deoxy-2'-α-fluoro-2'-β-C-methyluridine nucleoside were prepared and showed significant potency in the HCV subgenomic replicon assay (<1 μM) and produced high levels of triphosphate 6 in primary hepatocytes and in the livers of rats, dogs, and monkeys when administered in vivo. The single diastereomer 51 of diastereomeric mixture 14 was crystallized, and an X-ray structure was determined establishing the phosphoramidate stereochemistry as Sp, thus correlating for the first time the stereochemistry of a phosphoramidate prodrug with biological activity. 51 (PSI-7977) was selected as a clinical development candidate.

Published

2010

24. PSI-7851, a pronucleotide of beta-D-2'-deoxy-2'-fluoro-2'-C-methyluridine monophosphate, is a potent and pan-genotype inhibitor of hepatitis C virus replication.

Author

Lam AM, Murakami E, Espiritu C, Steuer HM, Niu C, Keilman M, Bao H, Zennou V, Bourne N, Julander JG, Morrey JD, Smee DF, Frick DN, Heck JA, Wang P, Nagarathnam D, Ross BS, Sofia MJ, Otto MJ, and Furman PA

Subjects

Amides chemistry, Amides pharmacology, Antiviral Agents chemistry, Cell Line, Tumor, Deoxyuracil Nucleotides chemistry, Enzyme Inhibitors chemistry, Genotype, Hepacivirus classification, Hepacivirus enzymology, Humans, Phosphoric Acids chemistry, Phosphoric Acids pharmacology, Prodrugs chemistry, RNA, Viral genetics, RNA, Viral metabolism, RNA-Dependent RNA Polymerase antagonists & inhibitors, Replicon drug effects, Viral Nonstructural Proteins antagonists & inhibitors, Antiviral Agents pharmacology, Deoxyuracil Nucleotides pharmacology, Enzyme Inhibitors pharmacology, Hepacivirus drug effects, Prodrugs pharmacology, Virus Replication drug effects

Abstract

The hepatitis C virus (HCV) NS5B RNA polymerase facilitates the RNA synthesis step during the HCV replication cycle. Nucleoside analogs targeting the NS5B provide an attractive approach to treating HCV infections because of their high barrier to resistance and pan-genotype activity. PSI-7851, a pronucleotide of beta-D-2'-deoxy-2'-fluoro-2'-C-methyluridine-5'-monophosphate, is a highly active nucleotide analog inhibitor of HCV for which a phase 1b multiple ascending dose study of genotype 1-infected individuals was recently completed (M. Rodriguez-Torres, E. Lawitz, S. Flach, J. M. Denning, E. Albanis, W. T. Symonds, and M. M. Berry, Abstr. 60th Annu. Meet. Am. Assoc. Study Liver Dis., abstr. LB17, 2009). The studies described here characterize the in vitro antiviral activity and cytotoxicity profile of PSI-7851. The 50% effective concentration for PSI-7851 against the genotype 1b replicon was determined to be 0.075+/-0.050 microM (mean+/-standard deviation). PSI-7851 was similarly effective against replicons derived from genotypes 1a, 1b, and 2a and the genotype 1a and 2a infectious virus systems. The active triphosphate, PSI-7409, inhibited recombinant NS5B polymerases from genotypes 1 to 4 with comparable 50% inhibitory concentrations. PSI-7851 is a specific HCV inhibitor, as it lacks antiviral activity against other closely related and unrelated viruses. PSI-7409 also lacked any significant activity against cellular DNA and RNA polymerases. No cytotoxicity, mitochondrial toxicity, or bone marrow toxicity was associated with PSI-7851 at the highest concentration tested (100 microM). Cross-resistance studies using replicon mutants conferring resistance to modified nucleoside analogs showed that PSI-7851 was less active against the S282T replicon mutant, whereas cells expressing a replicon containing the S96T/N142T mutation remained fully susceptible to PSI-7851. Clearance studies using replicon cells demonstrated that PSI-7851 was able to clear cells of HCV replicon RNA and prevent viral rebound.

Published

2010

25. Nucleoside analog inhibitors of hepatitis C viral replication: recent advances, challenges and trends.

Author

Furman PA, Lam AM, and Murakami E

Subjects

Hepatitis C, Chronic virology, Humans, Models, Molecular, Molecular Structure, Nucleosides metabolism, Ribavirin therapeutic use, Viral Nonstructural Proteins antagonists & inhibitors, Viral Nonstructural Proteins chemistry, Viral Nonstructural Proteins metabolism, Antiviral Agents chemistry, Antiviral Agents pharmacology, Antiviral Agents therapeutic use, Hepacivirus drug effects, Hepatitis C, Chronic drug therapy, Nucleosides chemistry, Virus Replication drug effects

Abstract

Chronic hepatitis C virus (HCV) infection is a global health problem, with over 170 million people infected worldwide. The current therapy, pegylated interferon (PEG-IFN) plus ribavirin (RBV), provides only approximately a 40% sustained virological response (undetectable HCV RNA for greater than 24 weeks after cessation of therapy), in genotype 1-infected individuals. In addition to the limited sustained virological response, PEG-IFN/RBV treatment is associated with serious adverse effects. Nucleosides have long been the cornerstone of antiviral therapy because of their proven efficacy and high barrier to resistance. Through the use of surrogate viruses or the HCV subgenomic replicon, several classes of nucleoside analogs or their monophosphate prodrugs have been identified that inhibit HCV RNA replication. Nucleoside analogs that possess the 2´-C-methyl modification vary in their ability to be phosphorylated and to act as alternative substrate inhibitors of the HCV RNA polymerase. Herein, we discuss various classes of nucleoside inhibitors, with a focus on available structure-activity relationships, their mode of action and resistance profile.

Published

2009

26. Understanding helicases as a means of virus control.

Author

Frick DN and Lam AM

Subjects

DNA Helicases chemistry, DNA Helicases physiology, DNA Primase antagonists & inhibitors, Papillomaviridae drug effects, Papillomaviridae enzymology, RNA Helicases chemistry, RNA Helicases physiology, Severe acute respiratory syndrome-related coronavirus drug effects, Severe acute respiratory syndrome-related coronavirus enzymology, Serine Endopeptidases, Simplexvirus drug effects, Simplexvirus enzymology, Viral Nonstructural Proteins antagonists & inhibitors, Viral Proteins antagonists & inhibitors, Antiviral Agents pharmacology, DNA Helicases antagonists & inhibitors, Enzyme Inhibitors pharmacology, RNA Helicases antagonists & inhibitors

Abstract

Helicases are promising antiviral drug targets because their enzymatic activities are essential for viral genome replication, transcription, and translation. Numerous potent inhibitors of helicases encoded by herpes simplex virus, severe acute respiratory syndrome coronavirus, hepatitis C virus, Japanese encephalitis virus, West Nile virus, and human papillomavirus have been recently reported in the scientific literature. Some inhibitors have also been shown to decrease viral replication in cell culture and animal models. This review discusses recent progress in understanding the structure and function of viral helicases to help clarify how these potential antiviral compounds function and to facilitate the design of better inhibitors. The above helicases and all related viral proteins are classified here based on their evolutionary and functional similarities, and the key mechanistic features of each group are noted. All helicases share a common motor function fueled by ATP hydrolysis, but differ in exactly how the motor moves the protein and its cargo on a nucleic acid chain. The helicase inhibitors discussed here influence rates of helicase-catalyzed DNA (or RNA) unwinding by preventing ATP hydrolysis, nucleic acid binding, nucleic acid release, or by disrupting the interaction of a helicase with a required cofactor.

Published

2006