Sex-based differences in natural killer T cell-mediated protection against diet-induced steatohepatitis in Balb/c mice

Carlos Cuño-Gómiz; Estefanía de Gregorio; Anna Tutusaus; Patricia Rider; Nuria Andrés-Sánchez; Anna Colell; Albert Morales; Montserrat Marí

doi:10.1186/s13293-023-00569-w

Biology of Sex Differences (Nov 2023)

Sex-based differences in natural killer T cell-mediated protection against diet-induced steatohepatitis in Balb/c mice

Carlos Cuño-Gómiz,
Estefanía de Gregorio,
Anna Tutusaus,
Patricia Rider,
Nuria Andrés-Sánchez,
Anna Colell,
Albert Morales,
Montserrat Marí

Affiliations

Carlos Cuño-Gómiz: Department of Cell Death and Proliferation, IIBB, CSIC, IDIBAPS
Estefanía de Gregorio: Department of Cell Death and Proliferation, IIBB, CSIC, IDIBAPS
Anna Tutusaus: Department of Cell Death and Proliferation, IIBB, CSIC, IDIBAPS
Patricia Rider: Department of Cell Death and Proliferation, IIBB, CSIC, IDIBAPS
Nuria Andrés-Sánchez: Institute of Molecular Genetics of Montpellier (IGMM), University of Montpellier, CNRS, INSERM
Anna Colell: Department of Cell Death and Proliferation, IIBB, CSIC, IDIBAPS
Albert Morales: Department of Cell Death and Proliferation, IIBB, CSIC, IDIBAPS
Montserrat Marí: Department of Cell Death and Proliferation, IIBB, CSIC, IDIBAPS

DOI: https://doi.org/10.1186/s13293-023-00569-w
Journal volume & issue: Vol. 14, no. 1
pp. 1 – 17

Abstract

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Abstract Background Metabolic dysfunction-associated steatotic liver disease (MASLD) is prevalent in Western countries, evolving into metabolic dysfunction-associated steatohepatitis (MASH) with a sexual dimorphism. Fertile women exhibit lower MASLD risk than men, which diminishes post-menopause. While NKT-cell involvement in steatohepatitis is debated, discrepancies may stem from varied mouse strains used, predominantly C57BL6/J with Th1-dominant responses. Exploration of steatohepatitis, encompassing both genders, using Balb/c background, with Th2-dominant immune response, and CD1d-deficient mice in the Balb/c background (lacking Type I and Type II NKT cells) can clarify gender disparities and NKT-cell influence on MASH progression. Methods A high fat and choline-deficient (HFCD) diet was used in male and female mice, Balb/c mice or CD1d−/− mice in the Balb/c background that exhibit a Th2-dominant immune response. Liver fibrosis and inflammatory gene expression were measured by qPCR, and histology assessment. NKT cells, T cells, macrophages and neutrophils were assessed by flow cytometry. Results Female mice displayed milder steatohepatitis after 6 weeks of HFCD, showing reduced liver damage, inflammation, and fibrosis compared to males. Male Balb/c mice exhibited NKT-cell protection against steatohepatitis whereas CD1d−/− males on HFCD presented decreased hepatoprotection, increased liver fibrosis, inflammation, neutrophilic infiltration, and inflammatory macrophages. In contrast, the NKT-cell role was negligible in early steatohepatitis development in both female mice, as fibrosis and inflammation were similar despite augmented liver damage in CD1d−/− females. Relevant, hepatic type I NKT levels in female Balb/c mice were significantly lower than in male. Conclusions NKT cells exert a protective role against experimental steatohepatitis as HFCD-treated CD1d−/− males had more severe fibrosis and inflammation than male Balb/c mice. In females, the HFCD-induced hepatocellular damage and the immune response are less affected by NKT cells on early steatohepatitis progression, underscoring sex-specific NKT-cell influence in MASH development.

Published in Biology of Sex Differences

ISSN: 2042-6410 (Online)
Publisher: BMC
Country of publisher: United Kingdom
LCC subjects: Medicine; Science: Physiology
Website: http://bsd.biomedcentral.com

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