| Literature DB >> 35881219 |
Hongzhi Liu1,2, Liang Li1, Yanyun Hao2, Jialu Li3, Zhaoyuan Liu1, Jingjing Qi1,4, Jingjing Zhang1, Ningbo Wu1, Dandan Wu1, Caixia Gao1, Lei Chen1, Lei Shen1, Jinke Cheng2, Bing Su5.
Abstract
Group 2 innate lymphoid cells (ILC2s) play important tissue resident roles in anti-parasite immunity, allergic immune response, tissue homeostasis, and tumor immunity. ILC2s are considered tissue resident cells with little proliferation at steady state. Recent studies have shown that a subset of small intestinal ILC2s could leave their residing tissues, circulate and migrate to different organs, including lung, liver, mesenteric LN and spleen, upon activation. However, it remains unknown whether other ILC populations with migratory behavior exist. In this study, we find two major colon ILC2 populations with potential to migrate to the lung in response to IL-25 stimulation. One subset expresses IL-17A and resembles inflammatory ILC2s (iILC2s) but lacks CD27 expression, whereas the other expresses CD27 but not IL-17A. In addition, the IL-17A+ ILC2s express lower levels of CD127, CD25, and ST2 than CD27+ ILC2s, which express higher levels of IL-5 and IL-13. Surprisingly, we found that both colon ILC2 populations still maintained their colonic features of preferential expression of IL-17A and CD27, IL-5/IL-13, respectively. Together, our study identifies two migratory colon ILC2 subsets with unique surface markers and cytokine profiles which are critical in regulating lung and colon immunity and homeostasis.Entities:
Keywords: CD27; IL-17A; ILC2s; colon; iILC2; lung inflammation
Year: 2022 PMID: 35881219 DOI: 10.1007/s11427-022-2127-2
Source DB: PubMed Journal: Sci China Life Sci ISSN: 1674-7305 Impact factor: 10.372