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正常的细胞周期进程需要 Groucho 在 S 期对 E2F1 进行负调控,并在 G2 期解除其调控。

Normal cell cycle progression requires negative regulation of E2F1 by Groucho during S phase and its relief at G2 phase.

机构信息

Department of Developmental Biology and Cancer Research, Institute for Medical Research Israel-Canada, Faculty of Medicine, The Hebrew University, Jerusalem 91120, Israel.

Department of Biological and Medical Sciences, Oxford Brookes University, Oxford OX3 0BP, UK.

出版信息

Development. 2023 Jun 1;150(11). doi: 10.1242/dev.201041.

Abstract

The cell cycle depends on a sequence of steps that are triggered and terminated via the synthesis and degradation of phase-specific transcripts and proteins. Although much is known about how stage-specific transcription is activated, less is understood about how inappropriate gene expression is suppressed. Here, we demonstrate that Groucho, the Drosophila orthologue of TLE1 and other related human transcriptional corepressors, regulates normal cell cycle progression in vivo. We show that, although Groucho is expressed throughout the cell cycle, its activity is selectively inactivated by phosphorylation, except in S phase when it negatively regulates E2F1. Constitutive Groucho activity, as well as its depletion and the consequent derepression of e2f1, cause cell cycle phenotypes. Our results suggest that Cdk1 contributes to phase-specific phosphorylation of Groucho in vivo. We propose that Groucho and its orthologues play a role in the metazoan cell cycle that may explain the links between TLE corepressors and several types of human cancer.

摘要

细胞周期依赖于一系列步骤,这些步骤通过特定阶段的转录物和蛋白质的合成和降解来触发和终止。尽管人们已经了解了如何激活阶段特异性转录,但对于如何抑制不适当的基因表达知之甚少。在这里,我们证明果蝇的 Groucho 与 TLE1 和其他相关的人类转录共抑制因子同源,它在体内调节正常的细胞周期进程。我们表明,尽管 Groucho 在整个细胞周期中都有表达,但它的活性除了在 S 期被磷酸化选择性失活外,还会负调控 E2F1。组成型的 Groucho 活性,以及其耗竭和随之而来的 e2f1 去抑制,导致细胞周期表型。我们的结果表明,Cdk1 有助于体内 Groucho 的阶段特异性磷酸化。我们提出,Groucho 及其同源物在后生动物细胞周期中发挥作用,这可能解释了 TLE 共抑制因子与多种人类癌症之间的联系。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/aa02/10281550/a5c2579a8f81/develop-150-201041-g1.jpg

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