240 Similar Adjusted Svr12 Rates for HIV Co-Infected and HCV Mono-Infected Patients and No Dose or Population (Treatment-Naïve/Relapser) Effect: Pooled Analysis of Faldaprevir Phase III Trials

Background: The efficacy of sofosbuvir (SOF)-containing regimens in patients who failed to achieve sustained virologic response (SVR) with SOF remains unknown. Given the lack of genotypic or phenotypic resistance to SOF in patients who did not achieve an SVR in the Phase 3 program, we designed an open-label study for relapsers to receive either a longer duration of SOF + RBV (24 weeks) or SOF + RBV with peginterferon (PEG-IFN). Methods: GT-2 and GT-3 HCV infected patients who failed either 12or 16-week regimens of SOF + RBV (Phase 3 studies: FISSION, FUSION, and POSITRON) were offered either 12-weeks of SOF (400 mg once daily) + PEG-IFN (180μg weekly) + RBV (1000-1200 mg daily) or an interferon-free 24-week arm of SOF+RBV. The choice of regimen was based upon investigator discretion. The primary efficacy endpoint is SVR12 and the secondary efficacy endpoint is SVR4. Results: A total of 97 GT-3 and 16 GT-2 patients have been enrolled. The majority of patients were male (80%) with a non-IL28CC genotype (65%) and 33% of patients had cirrhosis. To date, overall SVR4 rates are 96% (27/28) for GT-3 and 100% (6/ 6) for GT-2 infected patients. The table displays these data for patients who have reached the 4-week post-treatment visit. Conclusions: Retreatment with sofosbuvir regimens of longer duration or with the addition of PEG-IFN in prior SOF failures results in high SVR4 rates and appears to offer a viable approach for GT-2 or GT-3 HCV infected patients who fail to achieve an SVR with SOF+RBV regimens.