Hepatic C-X-C chemokine receptor type 6-expressing innate lymphocytes limit detrimental myeloid hyperactivation in acute liver injury

Felix Heymann; Jana C Mossanen; Moritz Peiseler; Patricia M Niemietz; Bruna Araujo David; Oliver Krenkel; Anke Liepelt; Matheus Batista Carneiro; Marlene S Kohlhepp; Paul Kubes; Frank Tacke

doi:10.1097/HC9.0000000000000102

Hepatic C-X-C chemokine receptor type 6-expressing innate lymphocytes limit detrimental myeloid hyperactivation in acute liver injury

Hepatol Commun. 2023 Mar 24;7(4):e0102. doi: 10.1097/HC9.0000000000000102. eCollection 2023 Apr 1.

Authors

Affiliations

¹ Department of Hepatology & Gastroenterology, Charité Universitätsmedizin Berlin, Campus Virchow Klinikum and Campus Charité Mitte, Berlin, Germany.
² Department of Intensive and Intermediate Care, University Hospital Aachen, Aachen, Germany.
³ Berlin Institute of Health (BIH), Berlin, Germany.
⁴ Department of Medicine III, University Hospital Aachen, Aachen, Germany.
⁵ Snyder Institute for Chronic Diseases, Cumming School of Medicine, University of Calgary, Calgary, Alberta, Canada.

Abstract

Background: Acute liver failure (ALF) is characterized by rapid clinical deterioration and high mortality. Acetaminophen (APAP or paracetamol) overdose is a leading cause of ALF, resulting in hepatocellular necrosis with subsequent inflammation, inflicting further liver damage. Infiltrating myeloid cells are early drivers of liver inflammation. However, the role of the abundant population of liver-resident innate lymphocytes, which commonly express the chemokine receptor CXCR6, is incompletely understood in ALF.

Methods: We investigated the role of CXCR6-expressing innate lymphocytes using the model of acute APAP toxicity in mice deficient in CXCR6 (Cxcr6gfp/gfp).

Results: APAP-induced liver injury was strongly aggravated in Cxcr6gfp/gfp mice compared with wild-type counterparts. Immunophenotyping using flow cytometry revealed a reduction in liver CD4+T cells, natural killer (NK) cells, and most prominently, NKT cells, whereas CXCR6 was dispensable for CD8+ T-cell accumulation. CXCR6-deficient mice exhibited excessive neutrophil and inflammatory macrophage infiltration. Intravital microscopy revealed dense cellular clusters of neutrophils in necrotic liver tissue, with higher numbers of clustering neutrophils in Cxcr6gfp/gfp mice. Gene expression analysis linked hyperinflammation in CXCR6 deficiency to increased IL-17 signaling. Although reduced in overall numbers, CXCR6-deficient mice had a shift in NKT cell subsets with increased RORγt-expressing NKT17 cells as a likely source of IL-17. In patients with ALF, we found a prominent accumulation of IL-17-expressing cells. Accordingly, CXCR6-deficient mice lacking IL-17 (Cxcr6gfp/gfpx Il17-/-) had ameliorated liver damage and reduced inflammatory myeloid infiltrates.

Conclusions: Our study identifies a crucial role of CXCR6-expressing liver innate lymphocytes as orchestrators in acute liver injury containing IL-17-mediated myeloid cell infiltration. Hence, strengthening the CXCR6-axis or downstream inhibition of IL-17 could yield novel therapeutics in ALF.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Acetaminophen / toxicity
Animals
Chemical and Drug Induced Liver Injury* / immunology
Inflammation
Interleukin-17*
Killer Cells, Natural
Mice
Receptors, CXCR6* / metabolism
T-Lymphocytes

Substances

Acetaminophen
Interleukin-17
Cxcr6 protein, mouse
Receptors, CXCR6