Direct, Competitive Comparison of Linear, Monocyclic, and Bicyclic Libraries Using mRNA Display

IF 4.3 3区 材料科学 Q1 ENGINEERING, ELECTRICAL & ELECTRONIC
David E. Hacker, Nicolas A. Abrigo, Jan Hoinka, Stacie L. Richardson, Teresa M. Przytycka, Matthew C. T. Hartman*
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引用次数: 10

Abstract

Peptide macrocyclization is typically associated with the development of higher affinity and more protease stable protein ligands, and, as such, is an important tool in peptide drug discovery. Yet, within the context of a diverse library, does cyclization give inherent advantages over linear peptides? Here, we used mRNA display to create a peptide library of diverse ring sizes and?topologies (monocyclic, bicyclic, and linear). Several rounds of in vitro selection against streptavidin were performed and the winning peptide sequences were analyzed for their binding affinities and overall topologies. The effect of adding a protease challenge on the enrichment of various peptides was also investigated. Taken together, the selection output yields insights about the relative abundance of binders of various topologies within a structurally diverse library.

Abstract Image

使用mRNA显示的线性、单环和双环文库的直接、竞争性比较
肽大环化通常与更高亲和力和更稳定的蛋白酶蛋白质配体的发展有关,因此是肽药物发现的重要工具。然而,在不同文库的背景下,环化是否具有优于线性肽的固有优势?在这里,我们使用mRNA展示来创建不同环大小的肽库。拓扑(单环、双环和线性)。进行了几轮体外抗链霉亲和素选择,并分析了获胜肽序列的结合亲和力和整体拓扑结构。研究了添加蛋白酶对不同多肽富集的影响。总的来说,选择输出产生关于结构多样的库中各种拓扑的粘合剂的相对丰度的见解。
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来源期刊
CiteScore
7.20
自引率
4.30%
发文量
567
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