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人类免疫缺陷病毒1型负调控因子(HIV-1 nef)与衔接蛋白复合物1、2和3的μ亚基的相互作用:基于双亮氨酸的分选基序的作用

Interactions of HIV-1 nef with the mu subunits of adaptor protein complexes 1, 2, and 3: role of the dileucine-based sorting motif.

作者信息

Craig H M, Reddy T R, Riggs N L, Dao P P, Guatelli J C

机构信息

Department of Pathology and, Department of Medicine, San Diego Veterans Affairs Medical Center, University of California at San Diego, 9500 Gilman Drive, La Jolla, California, 92093-0679, USA.

出版信息

Virology. 2000 May 25;271(1):9-17. doi: 10.1006/viro.2000.0277.

Abstract

HIV-1 Nef interacts with cellular adaptor protein (AP) complexes and their medium (mu) subunits. However, the role of the dileucine-based sorting motif within Nef in these interactions has been incompletely characterized. Here, yeast two-hybrid assays indicated that HIV-1 Nef interacted not only with the mu subunits of AP-1 and AP-2, but also with that of AP-3. The interactions with mu1 and mu3 were markedly stronger than the interaction with mu2. Leucine residues of the sorting motif were required for the interactions with mu3 and mu2 and contributed to the interaction with mu1. Confocal immunofluorescence microscopy indicated that Nef, AP-1, and AP-3 (but not AP-2) were concentrated in a juxtanuclear region near the cell center, potentially facilitating interaction between Nef and the mu1 and mu3 subunits. However, leucine residues of the sorting motif were not required for this subcellular localization of Nef. These data suggest that the dileucine motif, required for optimal viral replication, functions through interactions with a variety of AP complexes, including AP-3, potentially by recruiting adaptor complexes to subcellular locations specified by additional determinants in the Nef protein.

摘要

HIV-1 Nef与细胞衔接蛋白(AP)复合物及其μ亚基相互作用。然而,Nef中基于双亮氨酸的分选基序在这些相互作用中的作用尚未完全明确。在此,酵母双杂交试验表明,HIV-1 Nef不仅与AP-1和AP-2的μ亚基相互作用,还与AP-3的μ亚基相互作用。与μ1和μ3的相互作用明显强于与μ2的相互作用。分选基序的亮氨酸残基对于与μ3和μ2的相互作用是必需的,并且有助于与μ1的相互作用。共聚焦免疫荧光显微镜检查表明,Nef、AP-1和AP-3(而非AP-2)集中在细胞中心附近的近核区域,这可能促进了Nef与μ1和μ3亚基之间的相互作用。然而,分选基序的亮氨酸残基对于Nef的这种亚细胞定位并非必需。这些数据表明,对于最佳病毒复制所必需的双亮氨酸基序,通过与包括AP-3在内的多种AP复合物相互作用发挥功能,可能是通过将衔接复合物招募到Nef蛋白中其他决定簇指定的亚细胞位置来实现的。

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