通过β-硫代内酯介导的天然化学连接实现空间位阻较大的肽的偶联。

Coupling of sterically demanding peptides by β-thiolactone-mediated native chemical ligation.

作者信息

Chen Huan, Xiao Yunxian, Yuan Ning, Weng Jiaping, Gao Pengcheng, Breindel Leonard, Shekhtman Alexander, Zhang Qiang

机构信息

Department of Chemistry , University at Albany , State University of New York , 1400 Washington Avenue , Albany , NY 12222 , USA . Email:

State Key Laboratory of Natural and Biomimetic Drugs , School of Pharmaceutical Sciences , Peking University , 38 Xueyuan Road , Beijing 100191 , China.

出版信息

Chem Sci. 2018 Jan 23;9(7):1982-1988. doi: 10.1039/c7sc04744d. eCollection 2018 Feb 21.

DOI:10.1039/c7sc04744d

PMID:29675245

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC5892351/

Abstract

The ligation of sterically demanding peptidyl sites such as those involving Val-Val and Val-Pro linkages has proven to be extremely challenging with conventional NCL methods that rely on exogenous thiol additives. Herein, we report an efficient β-thiolactone-mediated additive-free NCL protocol that enables the establishment of these connections in good yield. The rapid NCL was followed by desulfurization. Reaction rates between β-thiolactones and conventional thioesters towards NCL were also investigated, and direct aminolysis was ruled out as a possible pathway. Finally, the potent cytotoxic cyclic-peptide axinastatin 1 has been prepared using the developed methodology.

摘要

事实证明，对于那些涉及缬氨酸-缬氨酸和缬氨酸-脯氨酸连接等空间位阻较大的肽基位点的连接，依靠外源性硫醇添加剂的传统天然化学连接（NCL）方法极具挑战性。在此，我们报告了一种高效的β-硫代内酯介导的无添加剂NCL方案，该方案能够以良好的产率建立这些连接。快速的NCL之后是脱硫。还研究了β-硫代内酯与传统硫酯对NCL的反应速率，并排除了直接氨解作为可能途径。最后，使用所开发的方法制备了具有强细胞毒性的环肽斧形他汀1。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/2a0f/5892351/3d5531b0a4b5/c7sc04744d-f1.jpg

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通过β-硫代内酯介导的天然化学连接实现空间位阻较大的肽的偶联。

Coupling of sterically demanding peptides by β-thiolactone-mediated native chemical ligation.

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