The median change in HCV RNA concentration from baseline to day 14 ranged from −3·7 to −5·2 log(10) IU/mL in the cohorts that received 13 days of combination treatment. At the highest combination doses tested (1000 mg RG7128 and 900 mg danoprevir twice daily), the median change in HCV RNA learn more concentration from baseline to day 14 was −5·1 log(10) IU/mL (IQR −5·6 to −4·7) in treatment-naive patients and −4·9 log(10) IU/mL in previous standard of care null responders (−5·2
to −4·5) compared with an increase of 0·1 log(10) IU/mL in the placebo group. The combination of RG7128 and danoprevir was well tolerated with no treatment-related serious or severe adverse events, no grade 3 or 4 changes in laboratory parameters, and no safety-related treatment discontinuations. Interpretation: This oral combination of a nucleoside analogue polymerase inhibitor and protease inhibitor holds promise as an interferon-free treatment for chronic HCV. Combination therapy with pegylated interferon (Peg-IFN)/ribavirin (RBV) has been Selleckchem Small molecule library the mainstay therapy of chronic hepatitis C virus (HCV) infection for the last decade.1 However, sustained virological response rates (SVR), which range from 40%-80%, vary considerably
with HCV genotypes. Genotype 1 is the most common genotype worldwide and has the lowest SVR rates (40%-50%) with 48 weeks of Peg-IFN/RBV therapy.1 However, not all patients are candidates for Peg-IFN/RBV therapies, and the multiple side effects associated with this therapy can be a major factor for lack of patient tolerance and treatment discontinuation. Thus, more effective and better tolerated therapies for individuals infected with genotype 1 are needed. Over the past
decade, predictors of SVR besides genotype have been identified that have allowed refinement of therapy; these include African American and Hispanic race, coinfection with human immunodeficiency virus, medchemexpress insulin resistance, viral level, and the recently identified interleukin-28B (IL-28) polymorphism. In addition to the above factors, the concept of response-guided therapy, whereby treatment duration is based on the rate of viral clearance from the serum during treatment, has allowed tailoring of therapy, allowing shorter duration of therapy in those who clear HCV RNA rapidly at week 4 (rapid virological response). Identification of the structural and nonstructural (NS) proteins of the hepatitis C genome has led to identification of targets to directly inhibit viral replication. The NS3/4A is a serine protease (NS3) and cofactor (NS4A) that catalyzes the posttranslational processing of NS proteins from the polyprotein that is essential for viral replication.2 The NS3 protease cleaves NS4A-NS4B, NS4B-NS5A, and NS5A-NS5B junctions.2 The products released go on to form a replicative complex responsible for forming viral RNA.
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