Innate lymphoid cells: More than just immune cells
Journal Title
Frontiers in Immunology
Abstract
Since their discovery, innate lymphoid cells (ILCs) have been described as the innate counterpart of the T cells. Indeed, ILCs and T cells share many features including their common progenitors, transcriptional regulation, and effector cytokine secretion. Several studies have shown complementary and redundant roles for ILCs and T cells, leaving open questions regarding why these cells would have been evolutionarily conserved. It has become apparent in the last decade that ILCs, and rare immune cells more generally, that reside in non-lymphoid tissue have non-canonical functions for immune cells that contribute to tissue homeostasis and function. Viewed through this lens, ILCs would not be just the innate counterpart of T cells, but instead act as a link between sensory cells that monitor any changes in the environment that are not necessarily pathogenic and instruct effector cells that act to maintain body homeostasis. As these non-canonical functions of immune cells are operating in absence of pathogenic signals, it opens great avenues of research for immunologists that they now need to identify the physiological cues that regulate these cells and how the process confers a finer level of control and a greater flexibility that enables the organism to adapt to changing environmental conditions. In the review, we highlight how ILCs participate in the physiologic function of the tissue in which they reside and how physiological cues, in particular neural inputs control their homeostatic activity.
Keywords
Il-22; Ilc1; Ilc2; Ilc3; gut homeostasis; metabolic homeostasis; neuroimmune interaction; physiological sensors
Research Division(s)
Immunology
PubMed ID
36389661
Open Access at Publisher's Site
https://doi.org/10.3389/fimmu.2022.1033904
Terms of Use/Rights Notice
Refer to copyright notice on published article.


Creation Date: 2022-12-13 03:13:12
Last Modified: 2022-12-14 01:17:12
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