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1型人类免疫缺陷病毒Nef蛋白选择性地与p21激活激酶2(PAK2)的具有催化活性的亚群结合,这一过程不依赖于PAK2与Nck或β-PIX的结合。

Human immunodeficiency virus type 1 Nef selectively associates with a catalytically active subpopulation of p21-activated kinase 2 (PAK2) independently of PAK2 binding to Nck or beta-PIX.

作者信息

Renkema G H, Manninen A, Saksela K

机构信息

Institute of Medical Technology, University of Tampere, Tampere, Finland.

出版信息

J Virol. 2001 Mar;75(5):2154-60. doi: 10.1128/JVI.75.5.2154-2160.2001.

Abstract

We have recently identified the Nef-associated serine-threonine kinase (NAK) as the p21-activated kinase 2 (PAK2). Here we have taken advantage of the possibility to manipulate the functional properties of NAK by transfecting PAK2 cDNA or its mutant derivatives in order to further characterize the Nef-NAK complex. To exclude the possibility that some Nef variants might interact with PAK1 instead of PAK2, we also examined the identity of NAK complexed with divergent human immunodeficiency virus type 1 HIV-1 Nef proteins. All tested Nef proteins, including SF2, NL4-3, BH10, and HAN-2, associated with PAK2 but not with PAK1. By exchanging different regions between these two PAK proteins, the selective ability of PAK2 to associate with Nef could be mapped to the carboxy-terminal part of its regulatory domain. Binding of PAK2 with the adapter protein Nck or beta-PIX was found to be dispensable for the assembly of the Nef-PAK2 complex, whereas an intact Cdc42-Rac1 interactive binding motif was required. Most importantly, we found that NAK represented a distinct subpopulation of the total cellular PAK2 characterized by a high specific kinase activity. Thus, although only a small fraction of cellular PAK2 could be found in complex with Nef, NAK represented a major part of cellular PAK2 activity.

摘要

我们最近鉴定出与Nef相关的丝氨酸 - 苏氨酸激酶(NAK)为p21激活激酶2(PAK2)。在此,我们利用转染PAK2 cDNA或其突变衍生物来操纵NAK功能特性的可能性,以进一步表征Nef - NAK复合物。为排除某些Nef变体可能与PAK1而非PAK2相互作用的可能性,我们还研究了与不同的1型人类免疫缺陷病毒(HIV - 1)Nef蛋白复合的NAK的身份。所有测试的Nef蛋白,包括SF2、NL4 - 3、BH10和HAN - 2,均与PAK2而非PAK1相关。通过交换这两种PAK蛋白之间的不同区域,PAK2与Nef结合的选择性能力可定位到其调节结构域的羧基末端部分。发现PAK2与衔接蛋白Nck或β - PIX的结合对于Nef - PAK2复合物的组装并非必需,而完整的Cdc42 - Rac1相互作用结合基序是必需的。最重要的是,我们发现NAK代表了总细胞PAK2中的一个独特亚群,其特征在于具有高特异性激酶活性。因此,尽管在与Nef形成复合物的细胞PAK2中仅能发现一小部分,但NAK代表了细胞PAK2活性的主要部分。

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