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RNAi 筛选端粒酶逆转录酶转录调控因子发现 HIF1alpha 对小鼠胚胎干细胞中端粒酶功能至关重要。

RNAi screen for telomerase reverse transcriptase transcriptional regulators identifies HIF1alpha as critical for telomerase function in murine embryonic stem cells.

机构信息

Institute for Biogenesis Research, University of Hawaii, Honolulu, HI 96813, USA.

出版信息

Proc Natl Acad Sci U S A. 2010 Aug 3;107(31):13842-7. doi: 10.1073/pnas.0913834107. Epub 2010 Jul 19.

Abstract

In various types of stem cells, including embryonic stem (ES) cells and hematopoietic stem cells, telomerase functions to ensure long-term self-renewal capacity via maintenance of telomere reserve. Expression of the catalytic component of telomerase, telomerase reverse transcriptase (Tert), which is essential for telomerase activity, is limiting in many types of cells and therefore plays an important role in establishing telomerase activity levels. However, the mechanisms regulating expression of Tert in cells, including stem cells, are presently poorly understood. In the present study, we sought to identify genes involved in the regulation of Tert expression in stem cells by performing a screen in murine ES (mES) cells using a shRNA expression library targeting murine transcriptional regulators. Of 18 candidate transcriptional regulators of Tert expression identified in this screen, only one candidate, hypoxia inducible factor 1 alpha (Hif1alpha), did not have a significant effect on mES cell morphology, survival, or growth rate. Direct shRNA-mediated knockdown of Hif1alpha expression confirmed that suppression of Hif1alpha levels was accompanied by a reduction in both Tert mRNA and telomerase activity levels. Furthermore, gradual telomere attrition was observed during extensive proliferation of Hif1alpha-targeted mES cells. Switching Hif1alpha-targeted mES cells to a hypoxic environment largely restored Hif1alpha levels, as well as Tert expression, telomerase activity levels, and telomere length. Together, these findings suggest a direct effect of Hif1alpha on telomerase regulation in mES cells, and imply that Hif1alpha may have a physiologically relevant role in maintenance of functional levels of telomerase in stem cells.

摘要

在各种类型的干细胞中,包括胚胎干细胞(ES 细胞)和造血干细胞,端粒酶通过维持端粒储备来确保长期的自我更新能力。端粒酶的催化成分端粒酶逆转录酶(Tert)的表达对于端粒酶活性是必不可少的,在许多类型的细胞中受到限制,因此在建立端粒酶活性水平方面发挥着重要作用。然而,目前对于调节细胞中 Tert 表达的机制,包括干细胞中的机制,了解甚少。在本研究中,我们通过使用针对小鼠转录调节剂的 shRNA 表达文库在小鼠胚胎干细胞(mES 细胞)中进行筛选,试图鉴定参与干细胞中 Tert 表达调节的基因。在该筛选中鉴定出的 18 个候选 Tert 表达的转录调节剂中,只有一个候选物,缺氧诱导因子 1 阿尔法(Hif1alpha),对 mES 细胞形态、存活或生长速率没有显著影响。直接 shRNA 介导的 Hif1alpha 表达抑制证实,Hif1alpha 水平的抑制伴随着 Tert mRNA 和端粒酶活性水平的降低。此外,在 Hif1alpha 靶向 mES 细胞的广泛增殖过程中观察到逐渐的端粒损耗。将 Hif1alpha 靶向 mES 细胞切换到低氧环境在很大程度上恢复了 Hif1alpha 水平,以及 Tert 表达、端粒酶活性水平和端粒长度。这些发现共同表明 Hif1alpha 对 mES 细胞中端粒酶调节的直接影响,并暗示 Hif1alpha 可能在维持干细胞中端粒酶的功能水平方面具有生理相关的作用。

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