Annals of Hepatology (Jul 2015)

High efficacy and safety of triple therapy in HCV genotype 1 and moderate fibrosis: a multicenter study of clinical practice in Spain

  • Javier Crespo, MD, Ph.D.,
  • Moisés Diago,
  • Joaquín Cabezas,
  • Marina Berenguer,
  • Teresa Broquetas,
  • Miguel Ángel Serra,
  • Rosa Morillas,
  • Javier García-Samaniego,
  • José Luis Calleja,
  • Juan José Sánchez,
  • Sabela Lens,
  • Susana Soto-Fernández,
  • Begoña Sacristán,
  • Inmaculada Fernández,
  • Carmen López-Núñez,
  • María Buti,
  • Manuel Romero-Gómez,
  • Federico Sáez-Royuela,
  • Conrado Fernández,
  • Francisco Jorquera,
  • Gloria Sánchez-Antolín,
  • Juan Manuel Pascasio,
  • Antonio Cuadrado,
  • Manuel Hernández-Guerra

Journal volume & issue
Vol. 14, no. 4
pp. 477 – 486

Abstract

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Background and rational. Telaprevir-based therapy (TBT) has been extensively evaluated in clinical trials. So we designed a study to compare the efficacy and safety of TBT between patients with moderate fibrosis and those suffering from advanced fibrosis in clinical practice. A multicenter observational and ambispective study was conducted. It included 582 patients with chronic hepatitis C genotype 1, 214 with fibrosis F2, and 368 with F3/F4 (F3: 148; F4: 220).Results. The mean patient age was 55 years, 67% male. Type of prior response was 22% naïve, 57% relapsers, and 21% partial/null responders, 69% had high viral load (> 800,000 IU/mL). HCV genotypes were 1a (19%), 1b (69%), and 1 (12%), respectively. Sixty-five percent were non-CC IL28B genotype. Week-12 sustained virologic response (SVR12) was significantly higher among F2-naïve patients (78%) compared with F3/F4-naïve patients (60%; p = 0.039) and among F2 non-responders (67%) compared with F3/F4 non-responders (42%; p = 0.014). SVR12 among relapsers was remarkably high in both groups (F2:89% vs. F3/F4:78%). Severe anemia and thrombocytopenia were more frequent among patients with F3/F4 than those with F2 (p < 0.01). Overall, 132 patients (22%) discontinued treatment: 58 due to adverse effects, 42 due to the stopping-rule, and 32 due to breakthrough. Premature discontinuation was more frequent among patients with F3/F4 (p = 0.028), especially due to breakthrough (p < 0.001). Conclusions. This multicenter study demonstrates high efficacy and an acceptable safety profile with regard to TBT in F2-patients in clinical practice.

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