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前沿:人类T淋巴细胞中的端粒酶激活并不需要端粒酶逆转录酶(hTERT)蛋白增加,但与hTERT磷酸化和核转位有关。

Cutting edge: telomerase activation in human T lymphocytes does not require increase in telomerase reverse transcriptase (hTERT) protein but is associated with hTERT phosphorylation and nuclear translocation.

作者信息

Liu K, Hodes R J

机构信息

Laboratory of Immunology, National Institute on Aging, National Institutes of Health, Baltimore, MD 21224, USA.

出版信息

J Immunol. 2001 Apr 15;166(8):4826-30. doi: 10.4049/jimmunol.166.8.4826.

Abstract

Capacity for cellular replication is critically important for lymphocyte function and can be regulated by telomerase-dependent maintenance of telomere length. In contrast to most normal human somatic cells that do not express telomerase due to the failure to transcribe telomerase reverse transcriptase (hTERT), lymphocytes express telomerase in a highly regulated fashion yet constitutively transcribe hTERT during development and activation. Here, we report that hTERT protein is present in both thymocytes and blood T cells at equivalent levels despite their substantial differences in telomerase activity, and that induction of telomerase activity in resting CD4(+) T cells is not dependent on net hTERT protein increase. Moreover, hTERT is phosphorylated and translocated from cytoplasm to nucleus during CD4(+) T cell activation. Thus, human T lymphocytes regulate telomerase function through novel events independent of hTERT protein levels, and hTERT phosphorylation and nuclear translocation may play a role in regulation of telomerase function in lymphocytes.

摘要

细胞复制能力对于淋巴细胞功能至关重要,并且可通过端粒酶依赖性的端粒长度维持来调节。与大多数正常人类体细胞因无法转录端粒酶逆转录酶(hTERT)而不表达端粒酶不同,淋巴细胞以高度调控的方式表达端粒酶,但在发育和激活过程中持续转录hTERT。在此,我们报告,尽管胸腺细胞和血液T细胞的端粒酶活性存在显著差异,但hTERT蛋白在二者中的含量相当,并且静息CD4(+) T细胞中端粒酶活性的诱导并不依赖于hTERT蛋白的净增加。此外,在CD4(+) T细胞激活过程中,hTERT发生磷酸化并从细胞质转位至细胞核。因此,人类T淋巴细胞通过独立于hTERT蛋白水平的新机制调节端粒酶功能,并且hTERT磷酸化和核转位可能在淋巴细胞端粒酶功能调节中发挥作用。

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