Assessment of HBV variants and novel viral and immune biomarkers in chronic hepatitis B patients with metabolic dysfunction associated steatotic liver disease

Author:

Patel Nishi H.12ORCID,Lucko Aaron12,Vachon Alicia3,Doucette Karen E.4,Ramji Alnoor5,Sycuro Laura2,Patel Trushar R.26ORCID,Chadee Kris2,Raman Maitreyi1,van Marle Guido2,Osiowy Carla3,Coffin Carla S.12ORCID

Affiliation:

1. Department of Medicine, Cumming School of Medicine University of Calgary Calgary Alberta Canada

2. Department of Microbiology, Immunology and Infectious Diseases, Cumming School of Medicine University of Calgary Calgary Alberta Canada

3. National Microbiology Laboratory Public Health Agency of Canada Winnipeg Manitoba Canada

4. Division of Infectious Diseases, Department of Medicine University of Alberta Edmonton Alberta Canada

5. Division of Gastroenterology, Department of Medicine University of British Columbia Vancouver British Columbia Canada

6. Departments of Chemistry and Biochemistry University of Lethbridge Lethbridge Alberta Canada

Abstract

AbstractCo‐existing chronic hepatitis B virus (CHB) infection and metabolic dysfunction associated steatotic liver disease (MASLD) can exert complex effects on hepatic metabolism, requiring mechanistic study. CHB participants were assessed for MASLD and the impact of hepatic steatosis/metabolic syndrome (MetS) on novel viral and immunological markers. In this prospective, cohort study, untreated CHB subjects were assessed for liver disease by non‐invasive tests (i.e. FibroScan, controlled attenuation parameter, CAP). Subjects were tested for cytokines and IFN‐γ ELISPOT assay to HBV Surface (S) and Core (C) proteins. Standard HBV serological, exploratory biomarkers and deep sequencing of HBV S and C genes were performed. In 53 subjects (median age 45 years [SD = 10.6], 35% F, 56% Asian, 20% Black, 3% White), 94% (50) HBeAg negative, 63% genotype B/C, mean HBV DNA 3.2 log10 IU/mL (SD = 1.8), quantitative HBsAg 2.9 log10 IU/mL (SD = 1.2) and HBV pgRNA 2.1 log10 copies/mL (SD = 1.3). In enrolled subjects, the mean ALT was 41.9 U/L (SD = 24.0), FibroScan was 5.7 kPa (SD = 1.9) and CAP was 306.4 dB/m (SD = 49.0). The mean BMI was 28.2 kg/m2 (SD = 4.2), 20% (11/53) had diabetes, 35% (19/53) dyslipidaemia and 24% (13/53) hypertension. Subjects with MetS and steatosis showed lower HBV markers (p < .01), higher HBV S diversity (p = .02) and greater frequency of HBV variants associated with host‐anti‐viral immune escape. Pro‐inflammatory cytokine levels and HBV‐specific cellular responses were higher in participants with hepatic steatosis. In CHB, MASLD/hepatic steatosis was associated with HBV variants and systemic immune responses potentially impacting liver disease progression despite low‐level viraemia.

Funder

Canadian Institutes of Health Research

GlaxoSmithKline Biologicals

Publisher

Wiley

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