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一种在哺乳动物冬眠期间理解p53转录调控的系统级方法。

A systems-level approach to understanding transcriptional regulation by p53 during mammalian hibernation.

作者信息

Pan Peipei, Treat Michael D, van Breukelen Frank

机构信息

School of Life Sciences, University of Nevada, Las Vegas, 4505 Maryland Parkway, Las Vegas, NV 89154, USA.

School of Life Sciences, University of Nevada, Las Vegas, 4505 Maryland Parkway, Las Vegas, NV 89154, USA

出版信息

J Exp Biol. 2014 Jul 15;217(Pt 14):2489-98. doi: 10.1242/jeb.103614.

Abstract

Presumably to conserve energy, many mammals enter into hibernation during the winter. Homeostatic processes such as transcription and translation are virtually arrested. To further elucidate transcriptional regulation during hibernation, we studied the transcription factor p53. Here, we demonstrate that changes in liver mRNA and protein concentrations of known regulators of p53 are consistent with activation. p53 mRNA and protein concentrations are unrelated. Importantly, p53 protein concentration is increased ~2-fold during the interbout arousal that punctuates bouts of torpor. As a result, both the interbout arousal and the torpid state are characterized by high levels of nuclear-localized p53. Chromatin immunoprecipitation assays indicate that p53 binds DNA during the winter. Furthermore, p53 recruits RNA polymerase II, as indicated by nuclear run-on data. However, and consistent with previous data indicating an arrest of transcriptional elongation during torpor, p53 'activity' does not result in expected changes in target gene transcripts. These data demonstrate the importance of using a systems level-approach in understanding a complex phenotype such as mammalian hibernation. Relying on interpretations of data that are based on steady-state regulation in other systems may be misleading in the context of non-steady-state conditions such as torpor.

摘要

据推测,许多哺乳动物为了保存能量,会在冬季进入冬眠状态。诸如转录和翻译等稳态过程几乎会停止。为了进一步阐明冬眠期间的转录调控,我们研究了转录因子p53。在此,我们证明,肝脏中已知的p53调节因子的mRNA和蛋白质浓度变化与激活一致。p53的mRNA和蛋白质浓度并无关联。重要的是,在打断蛰伏期的间歇性觉醒期间,p53蛋白质浓度增加了约2倍。因此,间歇性觉醒期和蛰伏状态均以高水平的核定位p53为特征。染色质免疫沉淀分析表明,p53在冬季会与DNA结合。此外,如核延伸数据所示,p53会募集RNA聚合酶II。然而,与之前表明蛰伏期间转录延伸停止的数据一致,p53的“活性”并未导致靶基因转录本出现预期变化。这些数据证明了采用系统水平方法来理解诸如哺乳动物冬眠这样的复杂表型的重要性。在诸如蛰伏这样的非稳态条件下,依赖基于其他系统中稳态调节的数据解释可能会产生误导。

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