Discovery of Small-Molecule Inhibitors of HCV NS3-4A Protease as Potential Therapeutic Agents against HCV Infection

Abstract: Chronic infection with hepatitis C virus (HCV) is associated with liver cirrhosis that often leads to hepatic failure and hepatocellular carcinoma (HCC). HCV infection has become a global health threat and the main cause of adult liver transplants in developed nations. Current approved anti-HCV therapies (interferon and pegylated interferon alone or in combination with ribavirin) are not effective in eliminating the viral infection in a significant population of patients (e.g., those infected with HCV genotype… Show more

“…The essential localization of this CARD domain-containing adapter to the mitochondria furthermore suggests an important function in the coordination of the innate immune and apoptotic responses. The implications for the study of HCV pathogenesis are particularly profound, given that experimental compounds, such as BILN2061 and VX-950, that block NS3-4A protease activity may accomplish two goals: inhibition of virus multiplication and processing and restoration of the early innate immune response that is critical to the development of a robust adaptive response in patients (9,22).…”

Dissociation of a MAVS/IPS-1/VISA/Cardif-IKKε Molecular Complex from the Mitochondrial Outer Membrane by Hepatitis C Virus NS3-4A Proteolytic Cleavage

“…The essential localization of this CARD domain-containing adapter to the mitochondria furthermore suggests an important function in the coordination of the innate immune and apoptotic responses. The implications for the study of HCV pathogenesis are particularly profound, given that experimental compounds, such as BILN2061 and VX-950, that block NS3-4A protease activity may accomplish two goals: inhibition of virus multiplication and processing and restoration of the early innate immune response that is critical to the development of a robust adaptive response in patients (9,22).…”

Dissociation of a MAVS/IPS-1/VISA/Cardif-IKKε Molecular Complex from the Mitochondrial Outer Membrane by Hepatitis C Virus NS3-4A Proteolytic Cleavage

“…Such resistance is well established in other viral diseases including HIV and HBV, and early data on HCV-active agents suggests that monotherapy has the potential to select early for key resistance mutations. 7 Regarding induction therapy, the committee agreed that monotherapy may be a feasible option if used as the first element of a sequential therapy plan. The rationale for this approach is that an induction phase to quickly lower the viral load prior to addition or substitution of an IFNbased regimen may enhance response rates and decrease the emergence of drug-resistant variants.…”

“…Both forms of mutation are highly relevant to new drug development, because binding site targeting may be genotype specific and emergence of site polymorphisms may lead to viral escape. 7 Chronic HCV infection leads to development of liver fibrosis in many but not all patients. Variable rates of fibrotic progression are described, and may be influenced by gender, age, and comorbidities including HIV coinfection, alcohol use, and presence of fatty liver (steatosis).…”

Development of novel agents for the treatment of chronic hepatitis C infection: Summary of the FDA Antiviral Products Advisory Committee recommendations

“…Specifically Targeted Antiviral Therapy against hepatitis C virus (STAT-C) stands for a new era in the treatment of patients with chronic hepatitis C. Various STAT-C compounds including boceprevir (SCH 503034) and telaprevir (VX 950) have already entered clinical trial phases. These compounds are blocking the NS3/4A protease of the hepatitis C virus which is located in the N-terminal domain of the HCV NS3 protein [3]. The NS3 protease is a serine protease essential for HCV polyprotein processing and therefore viral replication.…”

Highly sensitive determination of HCV protease inhibitors boceprevir (SCH 503034) and telaprevir (VX 950) in human plasma by LC–MS/MS