| Literature DB >> 33271118 |
Denis A Mogilenko1, Oleg Shpynov2, Prabhakar Sairam Andhey1, Laura Arthur1, Amanda Swain1, Ekaterina Esaulova1, Simone Brioschi1, Irina Shchukina1, Martina Kerndl3, Monika Bambouskova1, Zhangting Yao4, Anwesha Laha1, Konstantin Zaitsev5, Samantha Burdess1, Susan Gillfilan1, Sheila A Stewart4, Marco Colonna1, Maxim N Artyomov6.
Abstract
Systematic understanding of immune aging on a whole-body scale is currently lacking. We characterized age-associated alterations in immune cells across multiple mouse organs using single-cell RNA and antigen receptor sequencing and flow cytometry-based validation. We defined organ-specific and common immune alterations and identified a subpopulation of age-associated granzyme K (GZMK)-expressing CD8+ T (Taa) cells that are distinct from T effector memory (Tem) cells. Taa cells were highly clonal, had specific epigenetic and transcriptional signatures, developed in response to an aged host environment, and expressed markers of exhaustion and tissue homing. Activated Taa cells were the primary source of GZMK, which enhanced inflammatory functions of non-immune cells. In humans, proportions of the circulating GZMK+CD8+ T cell population that shares transcriptional and epigenetic signatures with mouse Taa cells increased during healthy aging. These results identify GZMK+ Taa cells as a potential target to address age-associated dysfunctions of the immune system.Entities:
Keywords: Aging; CD8 T cells; CITE-seq; granzyme K; immune system; inflammaging; single-cell ATAC-sequencing; single-cell BCR-sequencing; single-cell RNA-sequencing; single-cell TCR-sequencing
Year: 2020 PMID: 33271118 DOI: 10.1016/j.immuni.2020.11.005
Source DB: PubMed Journal: Immunity ISSN: 1074-7613 Impact factor: 31.745