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A novel approach for the identification of protein–protein interaction with integral membrane proteins

机译:一种新颖的识别方法 蛋白质与整合膜蛋白的相互作用

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摘要

Protein–protein interaction plays a major role in all biological processes. The currently available genetic methods such as the two-hybrid system and the protein recruitment system are relatively limited in their ability to identify interactions with integral membrane proteins. Here we describe the development of a reverse Ras recruitment system (reverse RRS), in which the bait used encodes a membrane protein. The bait is expressed in its natural environment, the membrane, whereas the protein partner (the prey) is fused to a cytoplasmic Ras mutant. Protein–protein interaction between the proteins encoded by the prey and the bait results in Ras membrane translocation and activation of a viability pathway in yeast. We devised the expression of the bait and prey proteins under the control of dual distinct inducible promoters, thus enabling a rapid selection of transformants in which growth is attributed solely to specific protein–protein interaction. The reverse RRS approach greatly extends the usefulness of the protein recruitment systems and the use of integral membrane proteins as baits. The system serves as an attractive approach to explore novel protein–protein interactions with high specificity and selectivity, where other methods fail.
机译:蛋白质之间的相互作用在所有生物过程中都起着重要作用。目前可用的遗传方法(例如双杂交系统和蛋白质募集系统)在识别与整合膜蛋白相互作用方面的能力相对有限。在这里,我们描述了反向Ras募集系统(reverse RRS)的发展,其中使用的诱饵编码膜蛋白。诱饵在其自然环境中的膜上表达,而蛋白伴侣(猎物)与细胞质Ras突变体融合。猎物和诱饵编码的蛋白质之间的蛋白质-蛋白质相互作用导致Ras膜易位并激活了酵母中的生存途径。我们设计了诱饵和猎物蛋白在双重截然不同的诱导型启动子控制下的表达,从而能够快速选择仅由于特定蛋白与蛋白相互作用而生长的转化子。反向RRS方法极大地扩展了蛋白质募集系统的用途以及将完整的膜蛋白用作诱饵的用途。该系统是吸引人的方法 探索具有高特异性的新型蛋白质间相互作用 和选择性,而其他方法则失败。

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