Long-term progression of viral load and serum markers of fibrosis among treated and untreated patients with chronic hepatitis B

Authors

Jia Li, Henry Ford HealthFollow
Stuart C. Gordon, Henry Ford HealthFollow
Loralee B. Rupp, Henry Ford HealthFollow
Talan Zhang, Henry Ford HealthFollow
Sheri Trudeau, Henry Ford HealthFollow
Scott D. Holmberg
Anne C. Moorman
Philip R. Spradling
Eyasu H. Teshale
Joseph A. Boscarino
Yihe G. Daida
Mark A. Schmidt
Mei Lu, Henry Ford HealthFollow

Recommended Citation

Li J, Gordon SC, Rupp LB, Zhang T, Trudeau S, Holmberg SD, Moorman AC, Spradling PR, Teshale EH, Boscarino JA, Daida YG, Schmidt MA, and Lu M. Long-term progression of viral load and serum markers of fibrosis among treated and untreated patients with chronic hepatitis B. J Gastroenterol Hepatol 2016;

Document Type

Article

Publication Date

6-1-2017

Publication Title

Journal of gastroenterology and hepatology

Abstract

BACKGROUND AND AIMS: Antiviral therapy for patients with hepatitis B (HBV) infection is generally deferred for "immune inactive" patients, although longitudinal changes in viral load and liver fibrosis remain understudied in this population. Likewise, in treated patients, the temporal relationship between changes in viral load and liver fibrosis is not well characterized. Using data from the chronic hepatitis cohort study, the study investigated viral load and the Fibrosis-4 index (FIB4, a serum-based marker of liver fibrosis) trajectories in both untreated and treated HBV patients.

MATERIALS AND METHODS: We applied a bivariate, piecewise, linear spline, mixed-effects modeling approach to data from 766 HBV patients (342 untreated, 424 treated). Treatment selection bias was adjusted using propensity scores. Multiple sensitivity analyses were used to confirm results in untreated patients.

RESULTS: Among all untreated patients, FIB4 began to increase by 0.9% per month (11% per year; P < 0.05) at 28 months post-index date, suggesting fibrosis progression. Significant FIB4 progression was also observed in a subgroup analysis of "immune inactive" untreated patients. In treated patients, viral load declined 31.8% per month (P < 0.05) for the first 5 months after treatment initiation, and 1.4-1.7% per month (P < 0.05) thereafter. At 5 months after treatment initiation, FIB4 began to decline 0.5% per month (P < 0.05), stabilizing at 28 months.

CONCLUSION: Among untreated HBV patients, FIB4 gradually increases over time, suggesting fibrosis progression, even in those patients designated as immune inactive. In treated patients, antiviral therapy results in a rapid decline in viral load followed by a delayed decline in markers of liver fibrosis.

Medical Subject Headings

Adult; Antiviral Agents; Biomarkers; Cohort Studies; Female; Fibrosis; Hepatitis B, Chronic; Humans; Liver; Male; Middle Aged; Time Factors; Viral Load

PubMed ID

27888529

Volume

32

Issue

6

First Page

1250

Last Page

1257