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p73 Alternative Splicing: Exploring a Biological Role for the C-Terminal Isoforms

机译:P73替代拼接:探索C末端同种型的生物学作用

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摘要

p73 (encoded by TP73 gene) is a p53 related protein that functions as a transcriptional factor. Similarly to p53, following DNA damage, p73 is stabilized and activated and controls expression of target genes that are involved in the regulation of cycle arrest and apoptosis. However, great complexity to the function of this gene is given by the wide range of its non-tumor-related roles, which include neurological development, ciliogenesis and fertility. From the structural point of view, p73 displays an intricate range of regulations because it can be expressed both as an N-terminally deleted dominant-negative isoforms and as multiple alternatively spliced C-terminal isoforms, which can include or not a sterile alpha motif domain. More is known about the functions of the N-terminal isoforms of p73 (TAp73 and Delta Np73) and their opposing pro-and anti-apoptotic roles, whereas the functional differences of the distinct C-terminal splice forms of p73 are very far away from been defined. Here we summarize the current available literature regarding p73 C-terminal isoforms and the contribution of the sterile alpha motif domain to p73 function, trying to provide an unified view in this complex and sometime controversial field. Current data indicate that the full-length, TAp73 alpha, is the major, if not the exclusive, isoform detected in physiological systems, indicating that detailed spatio-temporal expression analysis and functional studies are highly demanded to support a physiological role for the p73 alternative splicing. With this article, we also aim to emphasize the need to further investigation on the topic, refocusing the attention on what we believe are the most relevant unanswered questions. (C) 2018 The Author(s). Published by Elsevier Ltd.
机译:P73(由TP73基因编码)是一种用作转录因子的P53相关蛋白。与P53类似,在DNA损伤之后,P73稳定并激活并控制靶基因的表达,这些基因涉及循环骤停和细胞凋亡。然而,对该基因的功能的巨大复杂性是由其非肿瘤相关的作用的广泛提供,包括神经发育,纤毛生成和生育能力。从结构的角度来看,P73显示了复杂的规定范围,因为它可以表达为N-末端缺失的显性阴性同种型,并且与多个可拼接的C末端同种型同种型,这可以包括或不包括无菌α基序列。关于P73(TAP73和DELTA NP73)的N末端同种型的功能及其相反的亲和抗凋亡作用,而P73的不同C末端剪接形式的功能差异是非常遥远的已定义。在这里,我们总结了关于P73 C末端同种型的现有文献,以及无菌alpha主题域对P73功能的贡献,试图在该复合体和有时争议领域提供统一视图。目前的数据表明,全长TAP73α是主要的,如果不是在生理系统中检测到的独家同种型,表明详细的时空表达分析和功能性研究是非常需要支持P73替代品的生理作用拼接。通过本文,我们还旨在强调需要进一步调查该主题,从而重新关注我们认为是最相关的未答复问题。 (c)2018年作者。 elsevier有限公司出版

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