Phenotypic and Clonal Stability of Antigen-Inexperienced Memory-like T Cells across the Genetic Background, Hygienic Status, and Aging

抗原未接触过的记忆样T细胞的表型和克隆稳定性与遗传背景、卫生状况和衰老的关系

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作者:Alena Moudra ,Veronika Niederlova ,Jiri Novotny ,Lucie Schmiedova ,Jan Kubovciak ,Tereza Matejkova ,Ales Drobek ,Michaela Pribikova ,Romana Stopkova ,Dagmar Cizkova ,Ales Neuwirth ,Juraj Michalik ,Katerina Krizova ,Tomas Hudcovic ,Michal Kolar ,Hana Kozakova ,Jakub Kreisinger ,Pavel Stopka ,Ondrej Stepanek

Abstract

Ag-inexperienced memory-like T (AIMT) cells are functionally unique T cells, representing one of the two largest subsets of murine CD8+ T cells. However, differences between laboratory inbred strains, insufficient data from germ-free mice, a complete lack of data from feral mice, and an unclear relationship between AIMT cells formation during aging represent major barriers for better understanding of their biology. We performed a thorough characterization of AIMT cells from mice of different genetic background, age, and hygienic status by flow cytometry and multiomics approaches, including analyses of gene expression, TCR repertoire, and microbial colonization. Our data showed that AIMT cells are steadily present in mice, independent of their genetic background and hygienic status. Despite differences in their gene expression profiles, young and aged AIMT cells originate from identical clones. We identified that CD122 discriminates two major subsets of AIMT cells in a strain-independent manner. Whereas thymic CD122LOW AIMT cells (innate memory) prevail only in young animals with high thymic IL-4 production, peripheral CD122HIGH AIMT cells (virtual memory) dominate in aged mice. Cohousing with feral mice changed the bacterial colonization of laboratory strains but had only minimal effects on the CD8+ T cell compartment, including AIMT cells.

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