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The global prevalence and impact of steatotic liver disease and viral infections: A systematic review and meta-analysis.

  • 2025-04-14
  • Hepatology communications 9(5)
    • Jiajing Li
    • Jiahua Zhou
    • Pengfei Li
    • Yining Wang
    • Nathalie Ridderhof
    • Jaffar A Al-Tawfiq
    • Willem Pieter Brouwer
    • Kan Chen
    • Robert J de Knegt
    • Maikel P Peppelenbosch
    • Bettina E Hansen
    • Maarten F M Engel
    • Ming-Hua Zheng
    • Ziad A Memish
    • Mohammed Eslam
    • Harry L A Janssen
    • Qiuwei Pan
    • Ibrahim Ayada

Study Design

Type
Meta-Analysis
Population
viral-infected adult patients
Methods
systematically searched databases from inception to April 2, 2024, for observational studies recording viral-infected adult patients with eligible data on the presence of hepatic steatosis
Funding
Unclear

Background

Steatotic liver disease (SLD) affects ~30% of adults worldwide. The global population is continuously threatened by epidemic and endemic viral diseases. This study aims to thoroughly examine the interaction between SLD and major viral diseases.

Methods

We systematically searched databases from inception to April 2, 2024, for observational studies recording viral-infected adult patients with eligible data on the presence of hepatic steatosis.

Results

Six hundred thirty-six eligible studies were included in the analysis of SLD prevalence. Among patients with monoinfections, the highest SLD prevalence was observed in those infected with HCV at 49% (95% CI: 47%-51%), followed by SARS-CoV-2 (39%, 95% CI [34%-44%]), HIV (39%, 95% CI [33%-44%]), and HBV (36%, 95% CI [32%-40%]). Additionally, co-infections, such as HCV-HIV and HBV-HCV, exhibit even higher SLD prevalence. The prevalence of steatohepatitis is particularly high in HIV-infected (24%, 95% CI: 17%-30%) and HCV-infected (18%, 95% CI: 13%-24%) populations. The co-existence of SLD with viral infections was associated not only with the progression of liver disease but also with more severe outcomes of the infections and poorer responses to antiviral treatment. The combination of cardiometabolic risk factors and viral-associated and host factors contributes to the higher risk of SLD in viral-infected populations.

Conclusions

SLD is highly prevalent in viral-infected populations, and the reciprocal interactions between SLD and viral diseases exacerbate both conditions, leading to poorer patient outcomes in general.

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