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p21激活激酶1的核定位与染色质靶点

Nuclear localization and chromatin targets of p21-activated kinase 1.

作者信息

Singh Rajesh R, Song Chunying, Yang Zhibo, Kumar Rakesh

机构信息

Department of Molecular and Cellular Oncology, University of Texas M. D. Anderson Cancer Center, Houston, Texas 77030, USA.

出版信息

J Biol Chem. 2005 May 6;280(18):18130-7. doi: 10.1074/jbc.M412607200. Epub 2005 Mar 3.

DOI:10.1074/jbc.M412607200
PMID:15749698
Abstract

Pak1 (p21-activated kinase 1), a conserved, mammalian signaling kinase, is a downstream effector of small GTPases Rac1 and Cdc42 and of growth factor signaling. Until now, a major focus of study has been on the cytosolic functions of Pak1, where it is an important modulator of cytoskeletal reorganization, consequently playing a major role in cell survival, migration, and invasion. In this report, we demonstrate the nuclear localization of Pak1 upon stimulation by epidermal growth factor. Three nuclear localization signals (NLSs) were identified in the N-terminal domain of Pak1. With mutational analysis, the importance of each NLS was elucidated. Mutation of all three NLSs eliminated the nuclear localization of Pak1. Expression of Pak1 as a fusion protein with Gal4-DNA binding domain and Gal4-luciferase activity showed that Pak1 might increase transcription. To identify the potential targets of nuclear Pak1, we used a Pak1-specific chromatin immunoprecipitation-based screening assay and identified a series of Pak1-interacting target chromatins, including phosphofructokinase-muscle isoform (PFK-M) and nuclear factor of activated T-cell (NFAT1) genes. Pak1 associated with the upstream enhancer sequence and promoter of PFK-M and was involved in the stimulation of the PFK-M expression. It also associated with a portion of the NFAT1 gene and its upstream region, leading to the repression of NFAT1 expression. These investigations provide proof-of-principle evidence that Pak1 could influence the expression of its putative chromatin targets in both a positive and a negative manner. Together, for the first time, these findings defined the NLSs of the Pak1, its association with chromatin, and the resulting modulation of transcription, thus opening new avenues to further the search for nuclear Pak1 functions and identify putative Pak1-interacting nuclear proteins.

摘要

Pak1(p21活化激酶1)是一种保守的哺乳动物信号激酶,是小GTP酶Rac1和Cdc42以及生长因子信号传导的下游效应物。到目前为止,研究的主要重点一直是Pak1的胞质功能,它是细胞骨架重组的重要调节因子,因此在细胞存活、迁移和侵袭中发挥重要作用。在本报告中,我们证明了表皮生长因子刺激后Pak1的核定位。在Pak1的N端结构域中鉴定出三个核定位信号(NLS)。通过突变分析,阐明了每个NLS的重要性。所有三个NLS的突变消除了Pak1的核定位。将Pak1作为与Gal4-DNA结合结构域和Gal4-荧光素酶活性的融合蛋白表达表明,Pak1可能会增加转录。为了鉴定核Pak1的潜在靶点,我们使用了基于Pak1特异性染色质免疫沉淀的筛选试验,并鉴定出一系列与Pak1相互作用的靶染色质,包括磷酸果糖激酶-肌肉同工型(PFK-M)和活化T细胞核因子(NFAT1)基因。Pak1与PFK-M的上游增强子序列和启动子相关,并参与刺激PFK-M的表达。它还与NFAT1基因的一部分及其上游区域相关,导致NFAT1表达的抑制。这些研究提供了原理性证据,证明Pak1可以以正向和负向方式影响其假定的染色质靶点的表达。总之,这些发现首次确定了Pak1的NLS、其与染色质的关联以及由此产生的转录调节,从而为进一步探索核Pak1功能和鉴定假定的与Pak1相互作用的核蛋白开辟了新途径。

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