Nuevas terapias orales de acción directa para tratamiento de virus de hepatitis C (VHC).

Jose Ignacio Vargas; Juan Pablo Arab; Hugo Monrroy; Pilar Labbe; Valeska Sarmiento; Felipe Fuster; Francisco Barrera; Carlos Benítez; Marco Arrese; Francisco Fuster; Alejandro Soza

Autores/as

Jose Ignacio Vargas Departamento de Gastroenterología Facultad de Medicina Pontificia Universidad Católica de Chile.
Juan Pablo Arab Departamento de Gastroenterología Facultad de Medicina Pontificia Universidad Católica de Chile.
Hugo Monrroy Departamento de Gastroenterología Facultad de Medicina Pontificia Universidad Católica de Chile.
Pilar Labbe Departamento de Gastroenterología Facultad de Medicina Pontificia Universidad Católica de Chile.
Valeska Sarmiento Unidad de Hepatología Hospital Gustavo Fricke Viña del Mar
Felipe Fuster Unidad de Hepatología Hospital Gustavo Fricke Viña del Mar
Francisco Barrera Departamento de Gastroenterología Facultad de Medicina Pontificia Universidad Católica de Chile.
Carlos Benítez Departamento de Gastroenterología Facultad de Medicina Pontificia Universidad Católica de Chile.
Marco Arrese Departamento de Gastroenterología Facultad de Medicina Pontificia Universidad Católica de Chile.
Francisco Fuster Unidad de Hepatología Hospital Gustavo Fricke Viña del Mar
Alejandro Soza Departamento de Gastroenterología Facultad de Medicina Pontificia Universidad Católica de Chile.

Palabras clave:

Antiviral Agents, Chile, Drugs, Generic, Fibrosis, Hepatitis C, Latin America

Resumen

Background: The availability of direct-acting antivirals (DAA) for the treatment of chronic hepatitis C virus (HCV) infection is just starting to expand in Chile. Aim: To report the initial experience of patients treated with DAA and their evolution after treatment. Material and methods: Prospective cohort study, from June 2013 to August 2016 of patients treated with DAA for HCV in three clinical centers. The presence of cirrhosis, clinical and laboratory features; adverse events (AE) and post-treatment changes in liver function were evaluated. Sustained viral response at 12 weeks post-treatment (SVR12) was determined. Results: One hundred six patients aged 58 ± 13 years, 54% males, were included. HCV genotype 1b was present in 88% and 47% had cirrhosis. Treatment regimens were asunaprevir + daclatasvir (DCV) in 17% of patients, paritaprevir / ritonavir / ombitasvir + dasabuvir in 33%, sofosbuvir (SOF) + DCV in 19%, and SOF + ledipasvir in 30%. Twenty five percent of patients used generic drugs. SVR12 was 92.1%, with no differences between generic and brand-name drugs. Serious AE were recorded in 22% of patients, being more common in those with cirrhosis (34% vs 11.5%, p < 0.01). At 12 weeks post-treatment follow-up, there was a decrease in aminotransferase values (p <0.01), improvement in Child-Pugh score (5.9 vs. 5.5, p = 0.03) and decreased presence of ascites (p = 0.02). Conclusions: In our setting, DAA for HCV was highly effective and safe in non-cirrhotic patients. Hepatic function and inflammation improved at 12 weeks of follow-up. AE were common in patients with cirrhosis, suggesting that these patients should be treated by experienced teams. Generic drugs had similar effectiveness compared to originals.