2012
DOI: 10.1128/aac.00245-12
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TMC647055, a Potent Nonnucleoside Hepatitis C Virus NS5B Polymerase Inhibitor with Cross-Genotypic Coverage

Abstract: ABSTRACTHepatitis C virus (HCV) infection is a major global health burden and is associated with an increased risk of liver cirrhosis and hepatocellular carcinoma. There remains an unmet medical need for efficacious and safe direct antivirals with complementary modes of action for combination in treatment regimens to deliver a high cure rate with a short duration of treatment for HCV patients. Here we report thein vitroinhibitory activity, mode of act… Show more

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Cited by 40 publications
(28 citation statements)
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“…Emerging TMC647055 RAVs were found at time of failure in the majority of patients (in 14/17 and 2/5 patients with virologic failure in the 2- and 3-DAA regimens, respectively). These were observed at NS5B position 495 only, similar to the findings from in vitro TMC647055 selection experiments [11] and from the Phase 1b study that evaluated TMC647055 in monotherapy and in combination with SMV [12, 13]. There was no difference found in emerging RAVs between a low dose of TMC647055/RTV (450 mg QD; Panels 1–2) and a high dose (600 mg QD; Panel 3) or between HCV geno/subtypes.…”
Section: Discussionsupporting
confidence: 85%
“…Emerging TMC647055 RAVs were found at time of failure in the majority of patients (in 14/17 and 2/5 patients with virologic failure in the 2- and 3-DAA regimens, respectively). These were observed at NS5B position 495 only, similar to the findings from in vitro TMC647055 selection experiments [11] and from the Phase 1b study that evaluated TMC647055 in monotherapy and in combination with SMV [12, 13]. There was no difference found in emerging RAVs between a low dose of TMC647055/RTV (450 mg QD; Panels 1–2) and a high dose (600 mg QD; Panel 3) or between HCV geno/subtypes.…”
Section: Discussionsupporting
confidence: 85%
“…TMC647055 25 (Fig. 3), a nonzwitterionic 17-membered macrocyclic indole, has yielded potent and selective finger-loop inhibitors of the hepatitis C virus (HCV) NS5B polymerase [51]. Lead optimization from 20 to 25 in conjunction with in vivo evaluation in rats identified this compound showing nanomolar potency (EC 50 ¼ 77 nM) in HCV replicon cells, limited toxicity and offetarget activities, and encouraging preclinical pharmacokinetic profiles characterized by high liver distribution, and it is currently being evaluated in phase II clinical trials in combination with simeprevir [52].…”
Section: Indole Antiviral Agents: Drugs On Market or Compounds In CLImentioning
confidence: 99%
“…The next review in this series contains some extraordinary molecules as described by Siddappa, Shivaputra and Renukadevi Patil; (benz)imidazole‐and indole‐based macrocycles might seem terribly familiar but dicationic structures such as 12 are notably active against bacteria. [ ] Away from these exotic structures, the use of macrocycles in mainstream drug discovery is demonstrated by the clinical candidate TMC647055 13 , a potent inhibitor (77 n m ) of the NS5B polymerase from hepatitis C virus [ ] (Figure ).…”
Section: Comparison Of Lipinski Ro5 With Ppi Inhibitors and Macrocyclmentioning
confidence: 99%