Department of Chemistry, The Scripps Research Institute, 10550 N. Torrey Pines Road, La Jolla, CA, 92037, USA.
Angew Chem Int Ed Engl. 2018 Jul 9;57(28):8697-8701. doi: 10.1002/anie.201804885. Epub 2018 Jun 11.
Amino-γ-lactam (Agl) bridged dipeptides, commonly known as Freidinger lactams, have been shown to constrain peptide backbone topology and stabilize type II' β-turns. The utility of these links as peptide constraints has inspired new approaches to their incorporation into complex peptides and peptoids, all of which require harsh reaction conditions or protecting groups that limit their use on unprotected peptides and proteins. Herein, we employ a mild and selective alkylation of selenomethionine in acidic aqueous solution, followed by immobilization of the alkylated peptide on to bulk reverse-phase C silica and base-induced lactamization in DMSO. The utilization of selenomethionine, which is readily introduced by synthesis or expression, and the mild conditions enable selective backbone engineering in complex peptide and protein systems.
氨基-γ-内酰胺(Agl)桥连二肽,通常称为 Freidinger 内酰胺,已被证明可以约束肽骨架拓扑结构并稳定 II' 型β-转角。这些键作为肽约束的应用激发了将其引入复杂肽和肽类似物的新方法,所有这些方法都需要苛刻的反应条件或保护基团,这限制了它们在未保护的肽和蛋白质上的应用。在此,我们在酸性水溶液中采用硒代蛋氨酸的温和选择性烷基化,然后将烷基化肽固定在散装反相 C 硅胶上,并在 DMSO 中进行碱诱导内酰胺化。硒代蛋氨酸的使用,它可以通过合成或表达容易引入,以及温和的条件,使复杂肽和蛋白质系统中的选择性骨架工程成为可能。
