Efficacy and Safety of Danoprevir-Ritonavir plus Peginterferon Alfa-2a–Ribavirin in Hepatitis C Virus Genotype 1 Prior Null Responders | Zendy

Edward Gane | Zendy; Roman Rouzier | Zendy; Alicja WiercińskaDrapało | Zendy; Dominique Larrey | Zendy; Peter N. Morcos | Zendy; Barbara J. Brennan | Zendy; Sophie Le Pogam | Zendy; Isabel Nájera | Zendy; Rosemary Petric | Zendy; Jonathan Q. Tran | Zendy; Rohit Kulkarni | Zendy; Ying Zhang | Zendy; Patrick F. Smith | Zendy; Ellen S. Yetzer | Zendy; Nancy S. Shulman | Zendy

Open Access

Efficacy and Safety of Danoprevir-Ritonavir plus Peginterferon Alfa-2a–Ribavirin in Hepatitis C Virus Genotype 1 Prior Null Responders

Author(s) -

Edward Gane,

Roman Rouzier,

Alicja WiercińskaDrapało,

Dominique Larrey,

Peter N. Morcos,

Barbara J. Brennan,

Sophie Le Pogam,

Isabel Nájera,

Rosemary Petric,

Jonathan Q. Tran,

Rohit Kulkarni,

Ying Zhang,

Patrick F. Smith,

Ellen S. Yetzer,

Nancy S. Shulman

Publication year - 2013

Publication title -

antimicrobial agents and chemotherapy

Language(s) - English

Resource type - Journals

SCImago Journal Rank - 2.07

H-Index - 259

eISSN - 1070-6283

pISSN - 0066-4804

DOI - 10.1128/aac.01515-13

Subject(s) - ribavirin , ritonavir , virology , medicine , genotype , hepatitis c virus , gastroenterology , virus , biology , viral load , biochemistry , antiretroviral therapy , gene

Danoprevir (DNV) is a hepatitis C virus (HCV) protease inhibitor that achieves high sustained virologic response (SVR) rates in combination with peginterferon alfa-2a-ribavirin in treatment-naive HCV genotype 1 (G1)-infected patients. This study explored the efficacy and safety of ritonavir-boosted DNV (DNVr) plus peginterferon alfa-2a-ribavirin in G1-infected prior peginterferon-ribavirin null responders. Null responders (<2-log10 reduction in HCV RNA level at week 12) were given an open-label combination of 100 mg of ritonavir and 100 mg of DNV (100/100 mg DNVr) every 12 h (q12h) plus peginterferon alfa-2a-ribavirin for 12 weeks. All patients achieving an early virologic response (EVR; ≥2-log10 decrease in HCV RNA by week 12) continued treatment with peginterferon alfa-2a-ribavirin; those without an EVR discontinued all study drugs. Twenty-four prior null responders were enrolled; 16 patients (67%) were infected with HCV G1b, and 8 (33%) were infected with G1a. Ninety-six percent of patients had an IL28B non-CC genotype. A sustained virologic response at 24 weeks posttreatment (SVR24) was achieved in 67% of patients, with a higher rate in G1b-infected (88%) than G1a-infected (25%) patients. Resistance-related breakthrough occurred in 4/8 G1a and 1/16 G1b patients through the DNV resistance-associated variant (RAV) NS3 R155K. NS3 R155K was also detected in 2/2 G1a patients who relapsed. Treatment was well tolerated. Two patients withdrew prematurely from study medications due to adverse events. Two serious adverse events were reported; both occurred after completion of DNVr therapy and were considered unrelated to treatment. No grade 3 or 4 alanine aminotransferase (ALT) elevations were observed. DNVr plus peginterferon alfa-2a-ribavirin demonstrated high SVR24 rates in HCV G1b-infected prior null responders and was well tolerated. (This study has been registered at ClinicalTrials.gov under registration no. NCT01185860.).

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