Go to The Journal of Clinical Investigation
  • About
  • Editors
  • Consulting Editors
  • For authors
  • Publication ethics
  • Publication alerts by email
  • Transfers
  • Advertising
  • Job board
  • Contact
  • Physician-Scientist Development
  • Current issue
  • Past issues
  • By specialty
    • COVID-19
    • Cardiology
    • Immunology
    • Metabolism
    • Nephrology
    • Oncology
    • Pulmonology
    • All ...
  • Videos
  • Collections
    • In-Press Preview
    • Resource and Technical Advances
    • Clinical Research and Public Health
    • Research Letters
    • Editorials
    • Perspectives
    • Physician-Scientist Development
    • Reviews
    • Top read articles

  • Current issue
  • Past issues
  • Specialties
  • In-Press Preview
  • Resource and Technical Advances
  • Clinical Research and Public Health
  • Research Letters
  • Editorials
  • Perspectives
  • Physician-Scientist Development
  • Reviews
  • Top read articles
  • About
  • Editors
  • Consulting Editors
  • For authors
  • Publication ethics
  • Publication alerts by email
  • Transfers
  • Advertising
  • Job board
  • Contact
Role of MIF in coordinated expression of hepatic chemokines in patients with alcohol-associated hepatitis
Kyle L. Poulsen, Xiude Fan, Christopher D. Kibler, Emily Huang, Xiaoqin Wu, Megan R. McMullen, Lin Leng, Richard Bucala, Meritxell Ventura-Cots, Josepmaria Argemi, Ramon Bataller, Laura E. Nagy
Kyle L. Poulsen, Xiude Fan, Christopher D. Kibler, Emily Huang, Xiaoqin Wu, Megan R. McMullen, Lin Leng, Richard Bucala, Meritxell Ventura-Cots, Josepmaria Argemi, Ramon Bataller, Laura E. Nagy
View: Text | PDF
Research Article Hepatology Inflammation

Role of MIF in coordinated expression of hepatic chemokines in patients with alcohol-associated hepatitis

  • Text
  • PDF
Abstract

The chemokine system of ligands and receptors is implicated in the progression of alcohol-associated hepatitis (AH). Finding upstream regulators could lead to novel therapies. This study involved coordinated expression of chemokines in livers of healthy controls (HC) and patients with AH in 2 distinct cohorts of patients with various chronic liver diseases. Studies in cultured hepatocytes and in tissue-specific KO were used for mechanistic insight into a potential upstream regulator of chemokine expression in AH. Selected C-X-C chemokine members of the IL-8 chemokine family and C-C chemokine CCL20 were highly associated with AH compared with HC but not in patients with liver diseases of other etiologies (nonalcoholic fatty liver disease [NAFLD] and hepatitis C virus [HCV]). Our previous studies implicate macrophage migration inhibitory factor (MIF) as a pleiotropic cytokine/chemokine with the potential to coordinately regulate chemokine expression in AH. LPS-stimulated expression of multiple chemokines in cultured hepatocytes was dependent on MIF. Gao-binge ethanol feeding to mice induced a similar coordinated chemokine expression in livers of WT mice; this was prevented in hepatocyte-specific Mif–KO (MifΔHep) mice. This study demonstrates that patients with AH exhibit a specific, coordinately expressed chemokine signature and that hepatocyte-derived MIF might drive this inflammatory response.

Authors

Kyle L. Poulsen, Xiude Fan, Christopher D. Kibler, Emily Huang, Xiaoqin Wu, Megan R. McMullen, Lin Leng, Richard Bucala, Meritxell Ventura-Cots, Josepmaria Argemi, Ramon Bataller, Laura E. Nagy

×

Figure 5

Hepatocyte-specific Mif deletion prevents Gao-binge–induced hepatocellular injury, steatosis, and expression of the chemokine signature.

Options: View larger image (or click on image) Download as PowerPoint
Hepatocyte-specific Mif deletion prevents Gao-binge–induced hepatocellul...
Miffl/fl, C57BL/6, and MifΔHep mice were acclimated to a complete liquid diet and allowed free access to ethanol-containing (n = 5–6) or pair-fed (n = 4) control diets per Gao-binge feeding protocol. (A and B) Expression of Cxcl1, Lix, Ccl2, and Ccl20 chemokine mRNA (A) and expression of neutrophil markers Ly6G and Cxcr2 as well as monocyte surface marker Ccr2 mRNA (B) was determined by qPCR in mouse livers. (C) ALT (U/L) and AST (U/L) activity in circulation was determined in plasma, and hepatic triglyceride content was measured in liver homogenate. (D) Expression of ER stress–associated mRNA for spliced Xbp1 (sXbp1), Grp78, Chop, and Dr5 was determined in mouse liver by qPCR. Values are expressed as means ± SEM. P < 0.05 versus pair-fed controls within genotype, by 2-way ANOVA with least square means multiple comparison tests.

Copyright © 2026 American Society for Clinical Investigation
ISSN 2379-3708

Sign up for email alerts