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Insights into the Mechanism and Catalysis of Peptide Thioester Synthesis by Alkylselenols Provide a New Tool for Chemical Protein Synthesis

11 February 2021, Version 1
Working Paper
This content is an early or alternative research output and has not been peer-reviewed by Cambridge University Press at the time of posting.

Abstract

While thiol-based catalysts are widely employed for chemical protein synthesis relying on peptide thioester chemistry, this is less true for selenol-based catalysts whose development is in its infancy. In this study, we compared different selenols derived from the selenocysteamine scaffold for their capacity to promote thiol-thioester exchanges in water at mildly acidic pH and the production of peptide thioesters from bis(2-sulfanylethyl)amido (SEA) peptides. The usefulness of a selected selenol compound is illustrated by the total synthesis of a biologically active human chemotactic protein, which plays an important role in innate and adaptive immunity

Keywords

Chemical Protein Synthesis
selenol
Catalysis
Native Chemical Ligation
bis(2-sulfanylethyl)amido
selenocholine
selenocysteamine analogues
Chemotaxis assay
granulysin
Kinetic analysis
NCL chemistry
Selenoester
thiol-thioester exchange
acetoacetyl chemistry
Protein folding
disulfide bridges
SEA chemistry
One-Pot
cysteinyl peptides
peptide thioesters
Chemoselective

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Now Published

Insights into the Mechanism and Catalysis of Peptide Thioester Synthesis by Alkylselenols Provide a New Tool for Chemical Protein Synthesis [opens in a new tab]
Florent Kerdraon, Gemma Bogard, Benoît Snella, Hervé Drobecq, Muriel Pichavant, Vangelis Agouridas, Oleg Melnyk journal article
Molecules , Volume 26, Issue 5
Online publication date: Mar 04, 2021

Version History

Feb 11, 2021 Version 1

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The content is available under CC BY NC ND 4.0 [opens in a new tab]

DOI

10.26434/chemrxiv.13856942.v1
D O I: 10.26434/chemrxiv.13856942.v1 [opens in a new tab]

Funding

This work was supported by the CNRS, the University of Lille, the Pasteur Institute of Lille and by ANR grant ANR-18-CE44-0010

Author’s competing interest statement

The authors declare no conflict of interest

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