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通过进化研究 p53 异构体的生物学功能:来自动物和细胞模型的启示。

Biological functions of p53 isoforms through evolution: lessons from animal and cellular models.

机构信息

Centre for Oncology and Molecular Medicine, INSERM-European Associated Laboratory, University of Dundee, Ninewells Hospital, Dundee, Scotland, UK.

出版信息

Cell Death Differ. 2011 Dec;18(12):1815-24. doi: 10.1038/cdd.2011.120. Epub 2011 Sep 23.

Abstract

The TP53 tumour-suppressor gene is expressed as several protein isoforms generated by different mechanisms, including use of alternative promoters, splicing sites and translational initiation sites, that are conserved through evolution and within the TP53 homologues, TP63 and TP73. Although first described in the eighties, the importance of p53 isoforms in regulating the suppressive functions of p53 has only become evident in the last 10 years, by analogy with observations that p63 and p73 isoforms appeared indispensable to fully understand the biological functions of TP63 and TP73. This review summarizes recent advances in the field of 'p53 isoforms', including new data on p63 and p73 isoforms. Details of the alternative mechanisms that produce p53 isoforms and cis- and trans-regulators identified are provided. The main focus is on their biological functions (apoptosis, cell cycle, aging and so on) in cellular and animal models, including mouse, zebrafish and Drosophila. Finally, the deregulation of p53 isoform expression in human cancers is reviewed. Based on these latest results, several developments are expected in the future: the identification of drugs modulating p53 isoform expression; the generation of animal models and the evaluation of the use of p53 isoform as biomarkers in human cancers.

摘要

TP53 肿瘤抑制基因通过不同的机制表达为几种蛋白质异构体,包括使用不同的启动子、剪接位点和翻译起始位点,这些机制在进化过程中以及在 TP53 同源物 TP63 和 TP73 中是保守的。尽管 p53 异构体在调节 p53 的抑制功能方面的重要性在 10 年前才通过与 p63 和 p73 异构体的观察结果相类比而变得明显,但这些异构体对于充分理解 TP63 和 TP73 的生物学功能是不可或缺的。这篇综述总结了“p53 异构体”领域的最新进展,包括关于 p63 和 p73 异构体的新数据。提供了产生 p53 异构体的替代机制和鉴定的顺式和反式调节剂的详细信息。主要重点是它们在细胞和动物模型(包括小鼠、斑马鱼和果蝇)中的生物学功能(细胞凋亡、细胞周期、衰老等)。最后,综述了人类癌症中 p53 异构体表达的失调。基于这些最新结果,预计未来会有几个方面的发展:鉴定调节 p53 异构体表达的药物;生成动物模型和评估 p53 异构体作为人类癌症生物标志物的用途。

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