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T7 裂解性噬菌体展示肽库比 M13 丝状噬菌体展示肽库表现出更少的序列偏差。

T7 lytic phage-displayed peptide libraries exhibit less sequence bias than M13 filamentous phage-displayed peptide libraries.

作者信息

Krumpe Lauren R H, Atkinson Andrew J, Smythers Gary W, Kandel Andrea, Schumacher Kathryn M, McMahon James B, Makowski Lee, Mori Toshiyuki

机构信息

Basic Research Program, SAIC-Frederick, Inc., Frederick, MD, USA.

出版信息

Proteomics. 2006 Aug;6(15):4210-22. doi: 10.1002/pmic.200500606.

Abstract

We investigated whether the T7 system of phage display could produce peptide libraries of greater diversity than the M13 system of phage display due to the differing processes of lytic and filamentous phage morphogenesis. Using a bioinformatics-assisted computational approach, collections of random peptide sequences obtained from a T7 12-mer library (X(12)) and a T7 7-mer disulfide-constrained library (CX(7)C) were analyzed and compared with peptide populations obtained from New England BioLabs' M13 Ph.D.-12 and Ph.D.-C7C libraries. Based on this analysis, peptide libraries constructed with the T7 system have fewer amino acid biases, increased peptide diversity, and more normal distributions of peptide net charge and hydropathy than the M13 libraries. The greater diversity of T7-displayed libraries provides a potential resource of novel binding peptides for new as well as previously studied molecular targets. To demonstrate their utility, several of the T7-displayed peptide libraries were screened for streptavidin- and neutravidin-binding phage. Novel binding motifs were identified for each protein.

摘要

我们研究了由于裂解性噬菌体和丝状噬菌体形态发生过程不同,噬菌体展示的T7系统是否能产生比M13噬菌体展示系统具有更高多样性的肽库。使用生物信息学辅助的计算方法,对从T7 12聚体文库(X(12))和T7 7聚体二硫键约束文库(CX(7)C)获得的随机肽序列集合进行了分析,并与从新英格兰生物实验室的M13 Ph.D.-12和Ph.D.-C7C文库获得的肽群体进行了比较。基于此分析,与M13文库相比,用T7系统构建的肽库具有更少的氨基酸偏差、更高的肽多样性,以及更正常的肽净电荷和亲水性分布。T7展示文库的更高多样性为新的以及先前研究的分子靶点提供了新型结合肽的潜在资源。为了证明它们的实用性,对几个T7展示肽库进行了筛选,以寻找与链霉亲和素和中性链霉亲和素结合的噬菌体。为每种蛋白质鉴定了新的结合基序。

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