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Telomerase Activation and Rejuvenation of Telomere Length in Stimulated T Cells Derived from Serially Transplanted Hematopoietic Stem Cells

机译:连续移植造血干细胞衍生的受激T细胞中端粒酶激活和端粒长度的年轻化

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摘要

Telomeres shorten in hematopoietic cells, including hematopoietic stem cells (HSCs), during aging and after transplantation, despite the presence of readily detectable levels of telomerase in these cells. In T cells, antigenic stimulation has been shown to result in a marked increase in the level of telomerase activity. We now show that stimulation of T cells derived from serially transplanted HSC results in a telomerase-dependent elongation of telomere length to a size similar to that observed in T cells isolated directly from young mice. Southern analysis of telomere length in resting and anti-CD3/CD28 stimulated donor-derived splenic T cells revealed an increase in telomere size by ∼7 kb for the population as a whole. Stimulation of donor-derived T cells from recipients of HSCs from telomerase-deficient mice did not result in regeneration of telomere length, demonstrating a dependence on telomerase. Furthermore, clonal anti-CD3/CD28 stimulation of donor-derived T cells followed by fluorescent in situ hybridization (FISH) analysis of telomeric signal intensity showed that telomeres had increased in size by ∼50% for all clonal expansions. Together, these results imply that one role for telomerase in T cells may be to renew or extend replicative potential via the rejuvenation of telomere length.
机译:尽管在这些细胞中存在易于检测到的端粒酶水平,但在衰老期间和移植后,包括造血干细胞(HSC)在内的造血细胞中的端粒缩短。在T细胞中,抗​​原刺激已显示导致端粒酶活性水平显着提高。我们现在显示,对源自连续移植的HSC的T细胞的刺激导致端粒酶依赖的端粒长度延长,其大小类似于直接从年轻小鼠中分离的T细胞中观察到的大小。对静止的和抗CD3 / CD28刺激的供体来源的脾T细胞中端粒长度的Southern分析表明,整个群体的端粒大小增加了约7kb。端粒酶缺陷型小鼠的HSC受体从供体来源的T细胞的刺激不会导致端粒长度的再生,表明对端粒酶的依赖性。此外,克隆的抗CD3 / CD28刺激供体来源的T细胞,然后对端粒信号强度进行荧光原位杂交(FISH)分析,结果表明端粒的大小在所有克隆扩增中均增加了约50%。总之,这些结果暗示着端粒酶在T细胞中的一种作用可能是通过端粒长度的再生来更新或扩展复制潜能。

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