| Literature DB >> 29677387 |
Dominic Paquin-Proulx1, Benjamin C Greenspun1, Lise Pasquet2, Benedikt Strunz3, Soo Aleman4, Karolin Falconer4,5, Masaki Terabe2, Jay A Berzofsky2, Johan K Sandberg3, Espen Melum6,7,8, Douglas F Nixon1, Niklas K Björkström3.
Abstract
Innate lymphocytes are selectively enriched in the liver where they have important roles in liver immunology. Murine studies have shown that type I NKT cells can promote liver inflammation, whereas type II NKT cells have an anti-inflammatory role. In humans, type II NKT cells were found to accumulate in the gut during inflammation and IL13Rα2 was proposed as a marker for these cells. In the human liver, less is known about type I and II NKT cells. Here, we studied the phenotype and function of human liver T cells expressing IL13Rα2. We found that IL13Rα2 was expressed by around 1% of liver-resident memory T cells but not on circulating T cells. In support of their innate-like T-cell character, the IL13Rα2+ T cells had higher expression of promyelocytic leukaemia zinc finger (PLZF) compared to IL13Rα2- T cells and possessed the capacity to produce IL-22. However, only a minority of human liver sulfatide-reactive type II NKT cells expressed IL13Rα2. Collectively, these findings suggest that IL13Rα2 identifies tissue-resident intrahepatic T cells with innate characteristics and the capacity to produce IL-22.Entities:
Keywords: Human liver; IL-22; IL13Rα2; Innate T cells; PLZF
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Year: 2018 PMID: 29677387 PMCID: PMC6733416 DOI: 10.1002/eji.201747334
Source DB: PubMed Journal: Eur J Immunol ISSN: 0014-2980 Impact factor: 5.532