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DeltaNp53 或 p44:启动 p53 泵

DeltaNp53 or p44: priming the p53 pump.

作者信息

Scrable Heidi, Sasaki Tsutomu, Maier Bernhard

机构信息

Department of Neuroscience, University of Virginia, Room 6116, MR-4, Lane Road Extended, Charlottesville, VA 22908-1392, USA.

出版信息

Int J Biochem Cell Biol. 2005 May;37(5):913-9. doi: 10.1016/j.biocel.2004.11.014. Epub 2005 Jan 11.

Abstract

The human protein DeltaNp53 and its murine counterpart p44 are isoforms of the tumor suppressor p53 lacking the transactivation domain present in the first 39 (40 in mouse) amino acids of the full-length protein. This makes them similar in structure to the DeltaN isoforms of the other members of the p53 superfamily of transcription factors, p63 and p73. The principle way both the human and the murine proteins are generated is by alternative translation of the p53 mRNA utilizing a start site in exon 4. Choice of start site depends on an interaction between p53 and its cognate RNA. When the balance between DeltaNp53 (p44) and full-length p53 is altered, the function of p53 as a transcription factor is disturbed. One consequence of over-expressing p44 in mice is an acceleration of the aging process and altered expression of genes in the IGF-1 signaling cascade [Maier, B., Gluba, W., Bernier, B., Turner, T., Mohammad, K., Guise, T., et al. (2004). Modulation of mammalian lifespan by the short isoform of p53. Genes & Development, 18, 306-319]. This links p53 to the single most important growth factor pathway known to regulate lifespan in lower organisms.

摘要

人类蛋白质DeltaNp53及其小鼠对应物p44是肿瘤抑制因子p53的异构体,它们缺少全长蛋白质前39个(小鼠为40个)氨基酸中存在的反式激活结构域。这使得它们在结构上与转录因子p53超家族其他成员p63和p73的DeltaN异构体相似。人类和小鼠蛋白质产生的主要方式是通过利用外显子4中的起始位点对p53 mRNA进行可变翻译。起始位点的选择取决于p53与其同源RNA之间的相互作用。当DeltaNp53(p44)与全长p53之间的平衡发生改变时,p53作为转录因子的功能就会受到干扰。在小鼠中过表达p44的一个后果是加速衰老过程并改变IGF-1信号级联反应中基因的表达[迈尔,B.,格鲁巴,W.,伯尼尔,B.,特纳,T.,穆罕默德,K.,吉斯,T.等(2004年)。p53短异构体对哺乳动物寿命的调节。《基因与发育》,18,306 - 319]。这将p53与已知调节低等生物寿命的最重要的生长因子途径联系起来。

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