Recent studies using single-cell RNA sequencing technology have uncovered several subpopulations of CD4(+) T cells that accumulate with aging. These age-associated T cells are emerging as relevant players in the onset of inflammaging and tissue senescence. Here, based on information provided by single-cell RNA sequencing data, we present a flow cytometry panel that allows the identification of age-associated T cell subsets in systematic larger analysis in mice. We use this panel to evaluate at the single-cell level mitochondrial and senescence marks in the different age-associated CD4(+) T cell subpopulations. Our analysis identifies a subpopulation of regulatory T (T(reg)) cells that is characterized by the extracellular expression of the co-inhibitory molecule killer cell lectin-like receptor subfamily G member 1 (KLRG1) and accumulates with aging in humans and mice. KLRG1-expressing T(reg) cells display senescence features such as mitochondrial alterations, increased expression of cell-cycle regulators and genomic DNA damage. Functionally, KLRG1(+) T(reg) cells show a reduced suppressive activity in vivo accompanied by a pro-inflammatory phenotype.
KLRG1 identifies regulatory T cells with mitochondrial alterations that accumulate with aging.
KLRG1 可识别随着年龄增长而积累的线粒体改变的调节性 T 细胞
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作者:Soto-Heredero Gonzalo, Gabandé-RodrÃguez Enrique, Carrasco Elisa, Escrig-Larena José Ignacio, Gómez de Las Heras Manuel M, Delgado-Pulido Sandra, Francos-Quijorna Isaac, Blanco Eva M, Fernández-Almeida Ãlvaro, Abia David, RodrÃguez MarÃa Josefa, Fernández-DÃaz Cristina M, Ãlvarez-Flores MarÃa Beatriz, RamÃrez de Molina Ana, Jung Sascha, Del Sol Antonio, Zorita Virginia, Sánchez-Cabo Fátima, Torroja Carlos, Mittelbrunn MarÃa
| 期刊: | Nature Aging | 影响因子: | 19.400 |
| 时间: | 2025 | 起止号: | 2025 May;5(5):799-815 |
| doi: | 10.1038/s43587-025-00855-9 | 研究方向: | 细胞生物学 |
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