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Liver Fibrosis in Human Immunodeficiency Virus (HIV)-Hepatitis C Virus (HCV) Coinfection Before and After Sustained Virologic Response: What Is the Best Noninvasive Marker for Monitoring Regression?

Nadine Kronfli, Jim Young, Shouao Wang, Joseph Cox, Sharon Walmsley, Mark Hull, Curtis Cooper, Valérie Martel‐Laferrière, Alexander Wong, Neora Pick, Marina B. Klein, Canadian Coinfection Cohort Study Investigators, Lisa Barrett, Jeff Cohen, Brian Conway, Curtis Cooper, Pierre Côté, Joseph Cox, M. John Gill, Shariq Haider, Mark Hull, Marina B. Klein, Joan Montaner, Erica E. M. Moodie, Neora Pick, Anita Rachlis, Danielle Rouleau, Roger Sandre, Mark Tyndall, Steve Sanche, Marie-Louise Vachon, Sharon Walmsley, Alex Wong, David Wong

2020Clinical Infectious Diseases23 citationsDOIOpen Access PDF

Abstract

BACKGROUND: Noninvasive markers of liver fibrosis such as aspartate aminotransferase-to-platelet ratio (APRI) and transient elastography (TE) have largely replaced liver biopsy for staging hepatitis C virus (HCV). As there is little longitudinal data, we compared changes in these markers before and after sustained virologic response (SVR) in human immunodeficiency virus (HIV)-HCV coinfected patients. METHODS: Participants from the Canadian Coinfection Cohort study who achieved SVR after a first treatment with either interferon/ribavirin or direct acting antivirals (DAAs), with at least 1 pre- and posttreatment fibrosis measure were selected. Changes in APRI or TE (DAA era only) were modeled using a generalized additive mixed model, assuming a gamma distribution and adjusting for sex, age at HCV acquisition, duration of HCV infection, and time-dependent body mass index, binge drinking, and detectable HIV RNA. RESULTS: Of 1981 patients, 151 achieved SVR with interferon and 553 with DAAs; 94 and 382 met inclusion criteria, respectively. In the DAA era, APRI increased (0.03 units/year; 95% credible interval (CrI): -.05, .12) before, declined dramatically during, and then changed minimally (-0.03 units/year; 95% CrI: -.06, .01) after treatment. TE values, however, increased (0.74 kPa/year; 95% CrI: .36, 1.14) before treatment, changed little by the end of treatment, and then declined (-0.55 kPa/year; 95% CrI: -.80, -.31) after SVR. CONCLUSIONS: TE should be the preferred noninvasive tool for monitoring fibrosis regression following cure. Future studies should assess the risk of liver-related outcomes such as hepatocellular carcinoma according to trajectories of fibrosis regression measured using TE to determine if and when it will become safe to discontinue screening.

Topics & Concepts

MedicineCoinfectionHepatitis C virusInternal medicineTransient elastographyGastroenterologyHepatitis CHepatocellular carcinomaLiver biopsyRibavirinFibrosisCohortImmunologyBiopsyVirusHepatitis C virus researchLiver Disease Diagnosis and TreatmentLiver Disease and Transplantation
Liver Fibrosis in Human Immunodeficiency Virus (HIV)-Hepatitis C Virus (HCV) Coinfection Before and After Sustained Virologic Response: What Is the Best Noninvasive Marker for Monitoring Regression? | Litcius