Human innate lymphoid cells - 09/11/16

Doi : 10.1016/j.jaci.2016.09.009

Jenny Mjösberg, PhD ^a,^⁎ , Hergen Spits, PhD ^b
^a Center for Infectious Medicine, Department of Medicine Huddinge, Karolinska Institutet, Stockholm, Sweden
^b Department of Cell Biology and Histology, Academic Medical Center, University of Amsterdam, Amsterdam, The Netherlands

^∗Corresponding author: Jenny Mjösberg, PhD, Center for Infectious Medicine F59, Department of Medicine Huddinge, Karolinska Institutet, Karolinska University Hospital, 141 86 Stockholm, Sweden.Center for Infectious Medicine F59Department of Medicine HuddingeKarolinska InstitutetKarolinska University Hospital, 141 86 StockholmSweden

Abstract

Innate lymphoid cells (ILCs) are increasingly acknowledged as important mediators of immune homeostasis and pathology. ILCs act as early orchestrators of immunity, responding to epithelium-derived signals by expressing an array of cytokines and cell-surface receptors, which shape subsequent immune responses. As such, ILCs make up interesting therapeutic targets for several diseases. In patients with allergy and asthma, group 2 innate lymphoid cells produce high amounts of IL-5 and IL-13, thereby contributing to type 2–mediated inflammation. Group 3 innate lymphoid cells are implicated in intestinal homeostasis and psoriasis pathology through abundant IL-22 production, whereas group 1 innate lymphoid cells are accumulated in chronic inflammation of the gut (inflammatory bowel disease) and lung (chronic obstructive pulmonary disease), where they contribute to IFN-γ–mediated inflammation. Although the ontogeny of mouse ILCs is slowly unraveling, the development of human ILCs is far from understood. In addition, the growing complexity of the human ILC family in terms of previously unrecognized functional heterogeneity and plasticity has generated confusion within the field. Here we provide an updated view on the function and plasticity of human ILCs in tissue homeostasis and disease.

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Key words : Innate lymphoid cells, mucosal immunity, inflammatory bowel disease, allergy, asthma, psoriasis, tumor immunity, graft-versus-host disease

Abbreviations used : AD, ART, γc, CLP, cNK, COPD, CRSwNP, CRTH2, DC, FLG, GVHD, HSCT, ieILC1, ILC, ILC1, ILC2, ILC3, IL1R1, IL-2R, KLRG1, LN, LP, LT, LTi, Nfil3, NK, Nrp1, ROR, TLR, TSLP

Plan

Development, classification, heterogeneity, and redundancy of ILCs

Effector functions and plasticity of ILC subsets in tissues

ILCs in the formation of lymphoid organs: The function of LTi cells

ILCs in homeostasis, inflammation, and infection in the intestine

ILCs mediate inflammation in the respiratory system

ILCs mediate tissue repair and inflammation in the skin

ILCs mediate protection against GvHD

ILCs are depleted in patients with HIV but accumulate in those with filarial infections

Tissue-dependent roles for ILCs in tumor surveillance and rejection

Conclusions

Disclosure of potential conflict of interest: J. Mjösberg has received grants from the Swedish Society for Medical Research, the Knut and Alice Wallenberg Foundation, the Swedish Research Council, the Swedish Cancer Foundation, and the Swedish Foundation for Strategic Research and has consultant arrangements with ONO Pharmaceutical. H. Spits has received a grant from the European Research Council, has consultant arrangements with GlaxoSmithKline and Vaxxilon, is employed by and has patents and stock/stock options with AIMM Therapeutics, and has received royalties from the Netherland Cancer Institute.