All therapy should be discontinued if the HCV RNA level is ≥100 I

All therapy should be discontinued if the HCV RNA level is ≥100 IU/mL at week 12 or ≥10 to 15 IU/mL at week 24. Two phase 3 trials evaluated the efficacy of TVR in combination with PegIFN alfa-2a and RBV in treatment-naïve patients with

genotype 1 chronic HCV infection.16, 22 Black patients were included but not as a separate cohort and were insufficient in number to provide an adequate assessment of true response in this population. In the ADVANCE trial, patients received TVR together with PegIFN and RBV for either 8 (T8PR) or 12 (T12PR) weeks followed by GDC-0449 PegIFN and RBV alone in a response-guided paradigm.16 The TVR dose was 750 mg given by mouth every 8 hours with food (in particular, a fatty meal). Patients in the T8PR and T12PR groups who achieved an “extended RVR” (eRVR)—which for this drug was defined as undetectable (<10-15 IU/mL) HCV learn more RNA levels at weeks 4 and 12—stopped therapy at week 24, whereas those in whom an eRVR did not occur received a total of 48 weeks of PegIFN and RBV.

All patients in the control group received PegIFN and RBV therapy for 48 weeks. The overall SVR rates among patients in the T8PR and T12PR groups were 69% and 75%, respectively,16 compared with a rate of 44% in the control group (Table 2 and Fig. 3). Using the RGT approach, 58% and 57% of patients in the T12PR and T8PR groups, respectively, attained an eRVR, 89% and 83% of whom ultimately achieved an SVR.16 Thus, developing an eRVR appears to be the strongest predictor that an SVR will occur. SVR rates

were higher in TVR-containing regimens compared to SOC treatment among patients with disease characteristics found previously to be associated with a poorer response to SOC treatment. Although few black patients and other difficult-to-treat patient populations were included in the TVR phase 3 trials, an improved SVR rate was observed regardless of race, ethnicity, or level of hepatic fibrosis. With regard to race, treatment with a TVR-based regimen significantly improved find more SVR rates in black patients (T8PR, 58% and T12PR, 62%) compared to the SVR rates achieved in those treated with the SOC regimen (25%) (Fig. 3). Moreover, the SVR rate was >80% among black patients who achieved an eRVR on a TVR-based regimen. A total of 62% of patients in the T12PR group and 53% in the T8PR group with advanced fibrosis achieved an SVR, the rate improving to >80% among those with an eRVR. In the T12PR group, the impact of high versus low viral load (>800,000 or <800,000 IU/mL) on SVR rates was minimal; the SVR rate was 74% in patients with a high viral load and 78% in those with a low viral load. The ILLUMINATE trial focused on defining the utility of RGT in patients with an eRVR.

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