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捕获肽:β折叠与小分子之间的刚性连接。

Captides: rigid junctions between beta sheets and small molecules.

作者信息

Kier Brandon L, Andersen Niels H

机构信息

University of Washington - Chemistry, Bagley Hall Room 205 Box 351700, Seattle, WA, 98195-1700, USA.

出版信息

J Pept Sci. 2014 Sep;20(9):704-15. doi: 10.1002/psc.2657. Epub 2014 Jun 6.

Abstract

An extensive series of covalently linked small molecule-peptide adducts based on a terminally capped-beta hairpin motif is reported. The constructs can be prepared by standard solid-phase Fmoc chemistry with one to four peptide chains linked to small molecule hubs bearing carboxylic acid moieties. The key feature of interest is the precise, buried environment of the small molecule, and its rigid orientation relative to one or more short but fully structured peptide chain(s). Most of this study employs a minimalist nine residue 'captide', a capped β-turn, but we illustrate general applicability to peptides which can terminate in a beta strand. The non-peptide portion of these adducts can include nearly any molecule bearing one or more carboxylic acid groups. Fold-dependent rigidity sets this strategy apart from the currently available bioconjugation methods, which typically engender significant flexibility between peptide and tag. Applications to catalyst enhancement, drug design, higher-order assembly, and FRET calibration rulers are discussed.

摘要

报道了一系列基于末端封闭β-发夹基序的共价连接小分子-肽加合物。这些构建体可通过标准的固相Fmoc化学方法制备,其中一至四条肽链连接到带有羧酸基团的小分子中心。感兴趣的关键特征是小分子精确的埋藏环境,以及它相对于一条或多条短但结构完整的肽链的刚性取向。本研究大部分采用了简约的九残基“捕获肽”,即一个封闭的β-转角,但我们展示了其对可终止于β链的肽的普遍适用性。这些加合物的非肽部分几乎可以包括任何带有一个或多个羧酸基团的分子。折叠依赖性刚性使该策略有别于目前可用的生物缀合方法,后者通常在肽和标签之间产生显著的灵活性。讨论了其在催化剂增强、药物设计、高阶组装和FRET校准尺方面的应用。

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