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乙酰化的MyoD与CBP和/或p300的溴结构域之间的相互作用。

Interaction between acetylated MyoD and the bromodomain of CBP and/or p300.

作者信息

Polesskaya A, Naguibneva I, Duquet A, Bengal E, Robin P, Harel-Bellan A

机构信息

Laboratoire Oncogenèse, Différenciation et Transduction du Signal, CNRS UPR 9079, Institut André Lwoff, Villejuif, France.

出版信息

Mol Cell Biol. 2001 Aug;21(16):5312-20. doi: 10.1128/MCB.21.16.5312-5320.2001.

Abstract

Acetylation is emerging as a posttranslational modification of nuclear proteins that is essential to the regulation of transcription and that modifies transcription factor affinity for binding sites on DNA, stability, and/or nuclear localization. Here, we present both in vitro and in vivo evidence that acetylation increases the affinity of myogenic factor MyoD for acetyltransferases CBP and p300. In myogenic cells, the fraction of endogenous MyoD that is acetylated was found associated with CBP or p300. In vitro, the interaction between MyoD and CBP was more resistant to high salt concentrations and was detected with lower doses of MyoD when MyoD was acetylated. Interestingly, an analysis of CBP mutants revealed that the interaction with acetylated MyoD involves the bromodomain of CBP. In live cells, MyoD mutants that cannot be acetylated did not associate with CBP or p300 and were strongly impaired in their ability to cooperate with CBP for transcriptional activation of a muscle creatine kinase-luciferase construct. Taken together, our data suggest a new mechanism for activation of protein function by acetylation and demonstrate for the first time an acetylation-dependent interaction between the bromodomain of CBP and a nonhistone protein.

摘要

乙酰化作为一种核蛋白的翻译后修饰正在崭露头角,它对于转录调控至关重要,并且能改变转录因子与DNA结合位点的亲和力、稳定性和/或核定位。在此,我们展示了体外和体内的证据,表明乙酰化增加了成肌因子MyoD与乙酰转移酶CBP和p300的亲和力。在成肌细胞中,发现被乙酰化的内源性MyoD部分与CBP或p300相关联。在体外,当MyoD被乙酰化时,MyoD与CBP之间的相互作用对高盐浓度更具抗性,并且在较低剂量的MyoD时就能检测到。有趣的是,对CBP突变体的分析表明,与乙酰化MyoD的相互作用涉及CBP的溴结构域。在活细胞中,不能被乙酰化的MyoD突变体不与CBP或p300结合,并且在与CBP协同激活肌肉肌酸激酶 - 荧光素酶构建体的转录能力方面严重受损。综上所述,我们的数据提示了一种通过乙酰化激活蛋白质功能的新机制,并首次证明了CBP的溴结构域与非组蛋白之间存在乙酰化依赖性相互作用。

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