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通过与丝状噬菌体的主要外壳蛋白融合而高密度展示的新肽库的构建、利用和进化。

Construction, exploitation and evolution of a new peptide library displayed at high density by fusion to the major coat protein of filamentous phage.

作者信息

Iannolo G, Minenkova O, Gonfloni S, Castagnoli L, Cesareni G

机构信息

Department of Biology, University of Rome Tor Vergata, Italy.

出版信息

Biol Chem. 1997 Jun;378(6):517-21. doi: 10.1515/bchm.1997.378.6.517.

Abstract

The amino-terminus of the major coat protein (PVIII) of filamentous phage can be extended, up to 6-7 residues, without interfering with the phage life cycle. We have constructed a library of approximately ten millions different phage each displaying a different octapeptide joined to the amino-terminus of the 2700 copies of PVIII. Most of the resulting clones are able to produce infective particles. This molecular repertoire constituted by the periodic regular decoration of the phage filament surface, can be utilized to search elements that bind proteins or relatively small organic molecules like the textile dye Cibacron blue. By sequential growth cycles we have performed a library evolution experiment to select phage clones that have a growth advantage in the absence of any requirement for binding a specific target. The consensus of the best growers reveals a Pro rich sequence with large hydrophobic residues at position 7 and Asn at position 1 of the random peptide insert. We propose that the assembly secretion process is favoured in phages displaying this family of peptides since they fit the groove between two adjacent PVIII subunits by making advantageous molecular contacts on the phage surface.

摘要

丝状噬菌体主要外壳蛋白(PVIII)的氨基末端可以延长多达6 - 7个残基,而不会干扰噬菌体的生命周期。我们构建了一个约一千万种不同噬菌体的文库,每个噬菌体都展示一种与2700份PVIII的氨基末端相连的不同八肽。大多数所得克隆能够产生感染性颗粒。由噬菌体丝状表面的周期性规则修饰构成的这种分子库,可用于寻找能结合蛋白质或相对较小有机分子(如纺织染料汽巴蓝)的元件。通过连续的生长循环,我们进行了一项文库进化实验,以选择在不需要结合特定靶标的情况下具有生长优势的噬菌体克隆。最佳生长者的共有序列显示,在随机肽插入片段中,第7位有大的疏水残基且第1位为Asn的富含脯氨酸的序列。我们提出,展示这类肽的噬菌体有利于组装分泌过程,因为它们通过在噬菌体表面形成有利的分子接触来契合两个相邻PVIII亚基之间的凹槽。

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