AI Article Synopsis
- Innate lymphoid cells (ILCs) are specialized lymphocytes that don't have the diverse antigen receptors found in T and B cells, and they play crucial roles in maintaining tissue health.
- Over the last decade, research has shown that ILCs are not only involved in immune responses and inflammation but also contribute to metabolic balance, tissue remodeling, and interactions with the nervous system.
- Advances in understanding ILC biology have led to a re-evaluation of their classification, emphasizing their importance in various physiological processes such as tissue homeostasis and regeneration.
Article Abstract
Innate lymphoid cells (ILCs) are lymphocytes that do not express the type of diversified antigen receptors expressed on T cells and B cells. ILCs are largely tissue-resident cells and are deeply integrated into the fabric of tissues. The discovery and investigation of ILCs over the past decade has changed our perception of immune regulation and how the immune system contributes to the maintenance of tissue homeostasis. We now know that cytokine-producing ILCs contribute to multiple immune pathways by, for example, sustaining appropriate immune responses to commensals and pathogens at mucosal barriers, potentiating adaptive immunity, and regulating tissue inflammation. Critically, the biology of ILCs also extends beyond classical immunology to metabolic homeostasis, tissue remodeling, and dialog with the nervous system. The last 10 years have also contributed to our greater understanding of the transcriptional networks that regulate lymphocyte commitment and delineation. This, in conjunction with the recent advances in our understanding of the influence of local tissue microenvironments on the plasticity and function of ILCs, has led to a re-evaluation of their existing categorization. In this review, we distill the advances in ILC biology over the past decade to refine the nomenclature of ILCs and highlight the importance of ILCs in tissue homeostasis, morphogenesis, metabolism, repair, and regeneration.
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| http://dx.doi.org/10.1016/j.cell.2018.07.017 | DOI Listing |
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