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成体干细胞表现出 RNA 聚合酶 II 丝氨酸-2 磷酸化的全局抑制。

Adult stem cells exhibit global suppression of RNA polymerase II serine-2 phosphorylation.

机构信息

Ludwig Institute for Cancer Research, Nuffield Department of Clinical Medicine, University of Oxford, United Kingdom.

出版信息

Stem Cells. 2010 Sep;28(9):1571-80. doi: 10.1002/stem.476.

Abstract

Adult stem cells, which are characterized by their capacity for self-renewal and differentiation, participate in tissue homeostasis and response to injury. They are thought to enter a state of relative quiescence, known as reversible cell cycle arrest, but the underlying molecular mechanisms remain poorly characterized. Previous data from our laboratory has shown that housekeeping gene expression is downregulated in melanocyte stem cells (MelSCs), suggesting a global suppression of mRNA transcription. We now show, using antibodies against specific phosphorylated forms of RNA polymerase II (RNApII), that adult MelSCs do not undergo productive mRNA transcription elongation, while RNApII is activated and initialized, ready to synthesize mRNA upon stimulation, and that the RNApII kinase CDK9 is absent in adult MelSCs. Interestingly, other adult stem cells also, including keratinocyte, muscle, spermatogonia, and hematopoietic stem cells, showed a similar absence of RNApII phosphorylation. Although it is difficult to show the functional significance of this observation in vivo, CDK9 inhibition resulted in enhanced survival of cells that are deprived from survival factors. We conclude that the absence of productive mRNA transcription is an early, specific, and conserved characteristic of adult stem cells. Downregulation of mRNA transcription may lead to decreased rates of metabolism, and protection from cellular and genetic damage. Screening heterogeneous tissues, including tumors, for transcriptionally quiescent cells may result in the identification of cells with stem cell-like phenotypes.

摘要

成体干细胞的特征是自我更新和分化能力,参与组织稳态和对损伤的反应。它们被认为进入相对静止的状态,称为可逆细胞周期阻滞,但潜在的分子机制仍知之甚少。我们实验室之前的数据表明,管家基因的表达在黑素干细胞(MelSCs)中下调,这表明 mRNA 转录的全面抑制。我们现在使用针对 RNA 聚合酶 II(RNApII)特异性磷酸化形式的抗体表明,成体 MelSCs 不会进行有活力的 mRNA 转录延伸,而 RNApII 被激活并初始化,准备在受到刺激时合成 mRNA,并且 CDK9 激酶在成体 MelSCs 中缺失。有趣的是,其他成体干细胞,包括角质形成细胞、肌肉、精原细胞和造血干细胞,也表现出类似的 RNApII 磷酸化缺失。尽管很难在体内证明这种观察的功能意义,但 CDK9 抑制导致在剥夺生存因子的情况下细胞存活率提高。我们得出结论,有活力的 mRNA 转录缺失是成体干细胞的一个早期、特异和保守的特征。mRNA 转录的下调可能导致代谢率降低,并防止细胞和遗传损伤。对包括肿瘤在内的异质组织进行转录静止细胞的筛选可能导致具有干细胞样表型的细胞的鉴定。

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