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人类T细胞中的生长停滞由非编码RNA生长停滞特异性转录本5(GAS5)控制。

Growth arrest in human T-cells is controlled by the non-coding RNA growth-arrest-specific transcript 5 (GAS5).

作者信息

Mourtada-Maarabouni Mirna, Hedge Vanessa L, Kirkham Lucy, Farzaneh Farzin, Williams Gwyn T

机构信息

Institute for Science and Technology in Medicine, Huxley Building, Keele University, Keele, ST5 5BG, UK.

出版信息

J Cell Sci. 2008 Apr 1;121(Pt 7):939-46. doi: 10.1242/jcs.024646.

Abstract

The control of growth of lymphocyte populations is crucial to the physiological regulation of the immune system, and to the prevention of both leukaemic and autoimmune disease. This control is mediated through modulation of the cell cycle and regulation of cell death. During log-phase growth the rate of proliferation is high and there is a low rate of cell death. As the population density increases, the cell cycle is extended and apoptosis becomes more frequent as the population enters growth arrest. Here, we show that growth-arrest-specific transcript 5 (GAS5) plays an essential role in normal growth arrest in both T-cell lines and non-transformed lymphocytes. Overexpression of GAS5 causes both an increase in apoptosis and a reduction in the rate of progression through the cell-cycle. Consistent with this, downregulation of endogenous GAS5 inhibits apoptosis and maintains a more rapid cell cycle, indicating that GAS5 expression is both necessary and sufficient for normal growth arrest in T-cell lines as well as human peripheral blood T-cells. Control of apoptosis and the cell cycle by GAS5 has significant consequences for disease pathogenesis, because independent studies have already identified GAS5 as an important candidate gene in the development of autoimmune disease.

摘要

淋巴细胞群体生长的控制对于免疫系统的生理调节以及白血病和自身免疫性疾病的预防至关重要。这种控制是通过调节细胞周期和调控细胞死亡来介导的。在对数期生长期间,增殖速率高且细胞死亡率低。随着群体密度增加,细胞周期延长,并且当群体进入生长停滞时细胞凋亡变得更加频繁。在此,我们表明生长停滞特异性转录本5(GAS5)在T细胞系和未转化淋巴细胞的正常生长停滞中起重要作用。GAS5的过表达导致细胞凋亡增加以及细胞周期进程速率降低。与此一致,内源性GAS5的下调抑制细胞凋亡并维持更快的细胞周期,表明GAS5表达对于T细胞系以及人外周血T细胞的正常生长停滞既是必需的也是充分的。GAS5对细胞凋亡和细胞周期的控制对疾病发病机制具有重要影响,因为独立研究已经将GAS5鉴定为自身免疫性疾病发展中的一个重要候选基因。

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