抑制 CDK1-cyclin B 的激活：cUSP(7)上的 PP2A。

Restraining CDK1-cyclin B activation: PP2A on the cUSP(7).

机构信息

Cancer Early Detection Advanced Research Center, Knight Cancer Institute, Oregon Health & Science University, Portland, OR, USA.

Division of Oncological Sciences, Knight Cancer Institute, Oregon Health & Science University, Portland, OR, USA.

出版信息

EMBO J. 2021 Jun 1;40(11):e108486. doi: 10.15252/embj.2021108486. Epub 2021 May 10.

DOI:10.15252/embj.2021108486

PMID:33969907

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC8167361/

Abstract

USP7 inhibitors are gaining momentum as a therapeutic strategy to stabilize p53 through their ability to induce MDM2 degradation. However, these inhibitors come with an unexpected p53-independent toxicity, via an unknown mechanism. In this issue of The EMBO Journal, Galarreta et al report how inhibition of USP7 leads to re-distribution of PP2A from cytoplasm to nucleus and an increase of deleterious CDK1-dependent phosphorylation throughout the cell cycle, revealing a new regulatory mechanism for the progression of S-phase cells toward mitosis to maintain genomic integrity.

摘要

USP7 抑制剂通过诱导 MDM2 降解来稳定 p53，作为一种治疗策略正在逐渐受到关注。然而，这些抑制剂具有一种未知机制的意想不到的 p53 非依赖性毒性。在本期《EMBO 杂志》中，Galarreta 等人报告了 USP7 抑制剂如何导致 PP2A 从细胞质重新分布到细胞核，并增加整个细胞周期中有害的 CDK1 依赖性磷酸化，揭示了 S 期细胞向有丝分裂过渡以维持基因组完整性的新的调节机制。

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