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p21 - Cdc42/Rac 激活激酶(PAK)家族新成员的分子克隆

Molecular cloning of a new member of the p21-Cdc42/Rac-activated kinase (PAK) family.

作者信息

Manser E, Chong C, Zhao Z S, Leung T, Michael G, Hall C, Lim L

机构信息

Institute of Molecular and Cell Biology, National University of Singapore, Kent Ridge, Singapore.

出版信息

J Biol Chem. 1995 Oct 20;270(42):25070-8. doi: 10.1074/jbc.270.42.25070.

DOI:10.1074/jbc.270.42.25070
PMID:7559638
Abstract

A number of "target" proteins for the Rho family of small GTP-binding proteins have now been identified, including the protein kinases ACK and p65PAK (Manser, E., Leung, T., Salihuddin, H., Zhao, Z.-S., and Lim, L. (1994) Nature 367, 40-46). The purified serine/threonine kinase p65PAK has been shown to be directly activated by GTP-Rac1 or GTP-Cdc42. Here we report the cDNA sequence encoding a new brain-enriched PAK isoform beta-PAK, which shares 79% amino acid identity with the previously described alpha-isoform. Their mRNAs are differentially expressed in the brain, with alpha-PAK mRNA being particularly abundant in motor-associated regions. In vitro translation products of the alpha- and beta-PAK cDNAs exhibited relative molecular masses of 68,000 and 65,000, respectively, by SDS-polyacrylamide analysis. A specific beta-PAK peptide sequence was obtained from rat brain-purified p65PAK. Recombinant alpha- and beta-PAKs exhibited an increase in kinase activity mediated by GTP-p21 induced autophosphorylation. Cdc42 was a more potent activator in vitro of alpha-PAK kinase, and the fully activated enzyme is 300 times more active than the unphosphorylated form. Interestingly the down-regulation in the binding of p21s to recombinant beta-PAK and brain p65PAK, which is observed upon kinase activation does not occur with recombinant alpha-PAK.

摘要

现已鉴定出多种小GTP结合蛋白Rho家族的“靶”蛋白,包括蛋白激酶ACK和p65PAK(曼瑟,E.,梁,T.,萨利胡丁,H.,赵,Z.-S.,和林,L.(1994年)《自然》367卷,40 - 46页)。纯化的丝氨酸/苏氨酸激酶p65PAK已被证明可被GTP - Rac1或GTP - Cdc42直接激活。在此我们报告编码一种新的脑富集PAK同工型β - PAK的cDNA序列,它与先前描述的α - 同工型有79%的氨基酸同一性。它们的mRNA在脑中差异表达,α - PAK mRNA在运动相关区域特别丰富。通过SDS - 聚丙烯酰胺分析,α - 和β - PAK cDNA的体外翻译产物分别显示出相对分子质量为68,000和65,000。从大鼠脑纯化的p65PAK中获得了一个特定的β - PAK肽序列。重组α - 和β - PAKs表现出由GTP - p21诱导的自磷酸化介导的激酶活性增加。Cdc42在体外是α - PAK激酶更有效的激活剂,并且完全激活的酶比未磷酸化形式的活性高300倍。有趣的是,激酶激活后观察到的p21与重组β - PAK和脑p65PAK结合的下调在重组α - PAK中未发生。

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