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大脑大小的分子控制:神经干细胞生死的调节因子及其它。

Molecular control of brain size: regulators of neural stem cell life, death and beyond.

机构信息

Department of Oncology-Pathology, Cancer Centrum Karolinska (CCK), Karolinska Institutet, Stockholm, Sweden.

出版信息

Exp Cell Res. 2010 May 1;316(8):1415-21. doi: 10.1016/j.yexcr.2010.03.012. Epub 2010 Mar 19.

Abstract

The proper development of the brain and other organs depends on multiple parameters, including strictly controlled expansion of specific progenitor pools. The regulation of such expansion events includes enzymatic activities that govern the correct number of specific cells to be generated via an orchestrated control of cell proliferation, cell cycle exit, differentiation, cell death etc. Certain proteins in turn exert direct control of these enzymatic activities and thus progenitor pool expansion and organ size. The members of the Cip/Kip family (p21Cip1/p27Kip1/p57Kip2) are well-known regulators of cell cycle exit that interact with and inhibit the activity of cyclin-CDK complexes, whereas members of the p53/p63/p73 family are traditionally associated with regulation of cell death. It has however become clear that the roles for these proteins are not as clear-cut as initially thought. In this review, we discuss the roles for proteins of the Cip/Kip and p53/p63/p73 families in the regulation of cell cycle control, differentiation, and death of neural stem cells. We suggest that these proteins act as molecular interfaces, or "pilots", to assure the correct assembly of protein complexes with enzymatic activities at the right place at the right time, thereby regulating essential decisions in multiple cellular events.

摘要

大脑和其他器官的正常发育依赖于多个参数,包括特定祖细胞池的严格控制扩张。这种扩张事件的调节包括酶活性,通过协调控制细胞增殖、细胞周期退出、分化、细胞死亡等,来控制特定细胞的正确数量的产生。某些蛋白质反过来直接控制这些酶活性,从而控制祖细胞池的扩张和器官大小。Cip/Kip 家族(p21Cip1/p27Kip1/p57Kip2)成员是细胞周期退出的众所周知的调节剂,它们与细胞周期蛋白-CDK 复合物相互作用并抑制其活性,而 p53/p63/p73 家族的成员传统上与细胞死亡的调节有关。然而,很明显,这些蛋白质的作用并不像最初想象的那样明确。在这篇综述中,我们讨论了 Cip/Kip 和 p53/p63/p73 家族蛋白在神经干细胞的细胞周期控制、分化和死亡中的作用。我们认为这些蛋白质作为分子接口或“飞行员”,在正确的时间和地点确保具有酶活性的蛋白质复合物的正确组装,从而调节多个细胞事件中的重要决策。

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