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通过mRNA展示发现蛋白酶稳定肽的高度受限双环支架

Highly Constrained Bicyclic Scaffolds for the Discovery of Protease-Stable Peptides via mRNA Display.

作者信息

Hacker David E, Hoinka Jan, Iqbal Emil S, Przytycka Teresa M, Hartman Matthew C T

机构信息

Virginia Commonwealth University , Department of Chemistry, 1001 West Main Street, Richmond, Virginia 23284-2006, United States.

National Center for Biotechnology Information , 8600 Rockville Pike, Bethesda, Maryland 20894, United States.

出版信息

ACS Chem Biol. 2017 Mar 17;12(3):795-804. doi: 10.1021/acschembio.6b01006. Epub 2017 Feb 1.

Abstract

Highly constrained peptides such as the knotted peptide natural products are promising medicinal agents because of their impressive biostability and potent activity. Yet, libraries of highly constrained peptides are challenging to prepare. Here, we present a method which utilizes two robust, orthogonal chemical steps to create highly constrained bicyclic peptide libraries. This technology was optimized to be compatible with in vitro selections by mRNA display. We performed side-by-side monocyclic and bicyclic selections against a model protein (streptavidin). Both selections resulted in peptides with mid-nanomolar affinity, and the bicyclic selection yielded a peptide with remarkable protease resistance.

摘要

高度受限的肽,如打结肽天然产物,因其令人印象深刻的生物稳定性和强大的活性而成为有前景的药物。然而,制备高度受限的肽库具有挑战性。在此,我们提出一种方法,该方法利用两个稳健、正交的化学步骤来创建高度受限的双环肽库。该技术经过优化,可与通过mRNA展示进行的体外筛选兼容。我们针对一种模型蛋白(链霉亲和素)进行了单环和双环的平行筛选。两种筛选都产生了具有中纳摩尔亲和力的肽,并且双环筛选产生了一种具有显著蛋白酶抗性的肽。

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