Scientific Reports (Nov 2023)

Hepatocyte integrity depends on c-Jun-controlled proliferation in Schistosoma mansoni infected mice

  • Lukas Härle,
  • Verena von Bülow,
  • Lukas Knedla,
  • Frederik Stettler,
  • Heike Müller,
  • Daniel Zahner,
  • Simone Haeberlein,
  • Anita Windhorst,
  • Annette Tschuschner,
  • Monika Burg-Roderfeld,
  • Kernt Köhler,
  • Christoph G. Grevelding,
  • Elke Roeb,
  • Martin Roderfeld

DOI
https://doi.org/10.1038/s41598-023-47646-z
Journal volume & issue
Vol. 13, no. 1
pp. 1 – 13

Abstract

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Abstract Schistosomiasis is a parasitic disease affecting more than 250 million people worldwide. The transcription factor c-Jun, which is induced in S. mansoni infection-associated liver disease, can promote hepatocyte survival but can also trigger hepatocellular carcinogenesis. We aimed to analyze the hepatic role of c-Jun following S. mansoni infection. We adopted a hepatocyte-specific c-Jun knockout mouse model (Alb-Cre/c-Jun loxP) and analyzed liver tissue and serum samples by quantitative real-time PCR array, western blotting, immunohistochemistry, hydroxyproline quantification, and functional analyses. Hepatocyte-specific c-Jun knockout (c-JunΔli) was confirmed by immunohistochemistry and western blotting. Infection with S. mansoni induced elevated aminotransferase-serum levels in c-JunΔli mice. Of note, hepatic Cyclin D1 expression was induced in infected c-Junf/f control mice but to a lower extent in c-JunΔli mice. S. mansoni soluble egg antigen-induced proliferation in a human hepatoma cell line was diminished by inhibition of c-Jun signaling. Markers for apoptosis, oxidative stress, ER stress, inflammation, autophagy, DNA-damage, and fibrosis were not altered in S. mansoni infected c-JunΔli mice compared to infected c-Junf/f controls. Enhanced liver damage in c-JunΔli mice suggested a protective role of c-Jun. A reduced Cyclin D1 expression and reduced hepatic regeneration could be the reason. In addition, it seems likely that the trends in pathological changes in c-JunΔli mice cumulatively led to a loss of the protective potential being responsible for the increased hepatocyte damage and loss of regenerative ability.