Results from the exposure–response analysis suggest that increasing filibuvir doses beyond those tested in studies 1 and 2 is unlikely to result in greater reductions in HCV RNA concentrations. Based on the relationship observed for filibuvir dose and exposure (data HM781-36B clinical trial not shown), doses in excess of 200 mg BID are expected to achieve 24-hour
exposures resulting in at least half the maximal response, whereas doses in excess of 600 mg BID are expected to achieve exposures approaching the maximal response. A phase 2a study evaluating the effect of filibuvir given at 200, 300, and 500 mg BID (given for 4 weeks in combination with pegIFN and RBV) on HCV RNA concentrations showed that a greater proportion of patients achieved rapid virological response (>60%) at all filibuvir doses tested compared with the standard of care (0%).21 The exposure–response analysis, in conjunction with phase 2a combination study results, indicates that doses producing at least half the maximal response in monotherapy studies for filibuvir may be sufficient when used in combination with pegIFN Dabrafenib and RBV to improve efficacy compared with current standard-of-care therapy. Variants at NS5B residue 423 provided a clear correlate
of virologic breakthrough in these clinical studies (P. Troke, M. Lewis, P. Simpson, K. Gore, J. Hammond, C. Craig, M. Westby, unpublished data, 2010).22 This finding is consistent with in vitro
medchemexpress resistance data,16, 22 where high-level resistance has been demonstrated with variants (isoleucine, threonine, and valine) at residue 423. This finding is also consistent with data reported for other Thumb 2 NNIs. Specifically, variants at position 423 were identified via clonal sequence analysis as being the most predominant following VCH-759 exposure.23 There is no scientific rationale to expect that cross-resistance would occur between filibuvir and protease inhibitors and polymerase inhibitors that bind in other pockets in the polymerase protein.24 Several studies have been conducted to investigate the prevalence of known HCV drug-resistance mutations, including Met423Thr/Val/Ile, in the untreated HCV-infected patient population.25, 26 According to these studies, variants at position 423 are present in 2%-3% of the untreated patient population, and are associated with a reduction in the replicative fitness of the virus. The impact of pretreatment position 423 variants and/or the reduced fitness associated with these variants on response to therapy was not evaluated and is thus not yet understood. Although no position 423 variants were detected at baseline in either of the filibuvir monotherapy studies, a novel variant (Arg422Lys) was detected at baseline in virus isolated from a patient in study 1. This patient achieved a <0.