Literature DB >> 26982082

Internal Activation of Peptidyl Prolyl Thioesters in Native Chemical Ligation.

Yue Gui1, Lingqi Qiu1, Yaohao Li1, Hongxing Li1, Suwei Dong1.   

Abstract

Prolyl thioesters have shown significantly lower reactivities in native chemical ligation (NCL) in comparison to that of the alanyl thioester. This report describes a mild and efficient internal activation protocol of peptidyl prolyl thioesters in NCL without using any thiol-based additives, where the introduction of a 4-mercaptan substituent on the C-terminal proline significantly improves the reactivity of prolyl thioesters via the formation of a bicyclic thiolactone intermediate. The kinetic data indicate that the reaction rate is comparable to that of the reported data of alanyl thioesters, and the mechanistic studies suggest that the ligation of two peptide segments proceeds through an NCL-like pathway instead of a direct aminolysis, which ensures the chemoselectivity and compatibility of various amino acid side chains. This 4-mercaptoprolyl thioester-based protocol also allows an efficient one-pot ligation-desulfurization procedure. The utility of this method has been further demonstrated in the synthesis of a proline-rich region of Wilms tumor protein 1.

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Year:  2016        PMID: 26982082     DOI: 10.1021/jacs.6b01202

Source DB:  PubMed          Journal:  J Am Chem Soc        ISSN: 0002-7863            Impact factor:   15.419


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6.  Accelerated microfluidic native chemical ligation at difficult amino acids toward cyclic peptides.

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  6 in total

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