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通过组合鸟枪法扫描诱变获得的功能性蛋白质结合表位的不同观点。

Alternative views of functional protein binding epitopes obtained by combinatorial shotgun scanning mutagenesis.

作者信息

Pál Gábor, Fong Shun-Yin, Kossiakoff Anthony A, Sidhu Sachdev S

机构信息

Dept. of Biochemistry and Molecular Biology, Cummings Life Sciences Center, University of Chicago, IL 60637, USA.

出版信息

Protein Sci. 2005 Sep;14(9):2405-13. doi: 10.1110/ps.051519805.

Abstract

Combinatorial shotgun scanning mutagenesis was used to analyze two large, related protein binding sites to assess the specificity and importance of individual side chain contributions to binding affinity. The strategy allowed for cost-effective generation of a plethora of functional data. The ease of the technology promoted comprehensive investigations, in which the classic alanine-scanning approach was expanded with two additional strategies, serine- and homolog-scanning. Binding of human growth hormone (hGH) to the hGH receptor served as the model system. The entire high affinity receptor-binding sites (site 1) of wild-type hGH (hGHwt) and of an affinity-improved variant (hGHv) were investigated and the results were compared. The contributions that 35 residue positions make to binding were assessed on each hormone molecule by both serine- and homolog-scanning. The hormone molecules were displayed on the surfaces of bacteriophage, and the 35 positions were randomized simultaneously to allow equal starting frequencies of the wild-type residue and either serine or a homologous mutation in separate libraries. Functional selections for binding to the hGH receptor shifted the relative wild-type/mutant frequencies at each position to an extent characteristic of the functional importance of the side chain. Functional epitope maps were created and compared to previous maps obtained by alanine-scanning. Comparisons between the different scans provide insights into the affinity maturation process that produced hGHv. The serine and homolog-scanning results expand upon and complement the alanine-scanning results and provide additional data on the robustness of the high affinity receptor-binding site of hGH.

摘要

组合鸟枪法扫描诱变用于分析两个大的相关蛋白质结合位点,以评估单个侧链对结合亲和力贡献的特异性和重要性。该策略能够经济高效地生成大量功能数据。该技术的简便性促进了全面研究,其中经典的丙氨酸扫描方法通过另外两种策略(丝氨酸扫描和同源物扫描)得到扩展。人生长激素(hGH)与hGH受体的结合作为模型系统。研究了野生型hGH(hGHwt)和亲和力提高变体(hGHv)的整个高亲和力受体结合位点(位点1),并比较了结果。通过丝氨酸扫描和同源物扫描在每个激素分子上评估了35个残基位置对结合的贡献。激素分子展示在噬菌体表面,35个位置同时随机化,以在单独的文库中允许野生型残基与丝氨酸或同源突变具有相等的起始频率。与hGH受体结合的功能选择将每个位置的相对野生型/突变频率转移到侧链功能重要性所特有的程度。创建了功能表位图谱,并与先前通过丙氨酸扫描获得的图谱进行比较。不同扫描之间的比较为产生hGHv的亲和力成熟过程提供了见解。丝氨酸和同源物扫描结果扩展并补充了丙氨酸扫描结果,并提供了关于hGH高亲和力受体结合位点稳健性的额外数据。

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