2,2 '-Dipyridyl diselenide: A chemoselective tool for cysteine deprotection and disulfide bond formation | Health & Environmental Research Online (HERO)

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Citation
Tags

HERO ID

7129517

Reference Type

Journal Article

Title

2,2 '-Dipyridyl diselenide: A chemoselective tool for cysteine deprotection and disulfide bond formation

Author(s)

Stemarie, EJ; Hondal, RJ; ,

Year

2019

Is Peer Reviewed?

Yes

Journal

Journal of Peptide Science
ISSN: 1075-2617

Publisher

WILEY

Location

HOBOKEN

Volume

Issue

Page Numbers

e3236

Language

English

PMID

31856422

DOI

10.1002/psc.3236

Web of Science Id

WOS:000503351900001

Abstract

There are many examples of bioactive, disulfide-rich peptides and proteins whose biological activity relies on proper disulfide connectivity. Regioselective disulfide bond formation is a strategy for the synthesis of these bioactive peptides, but many of these methods suffer from a lack of orthogonality between pairs of protected cysteine (Cys) residues, efficiency, and high yields. Here, we show the utilization of 2,2 '-dipyridyl diselenide (PySeSePy) as a chemical tool for the removal of Cys-protecting groups and regioselective formation of disulfide bonds in peptides. We found that peptides containing either Cys(Mob) or Cys(Acm) groups treated with PySeSePy in trifluoroacetic acid (TFA) (with or without triisopropylsilane (TIS) were converted to Cys-S-SePy adducts at 37 degrees C and various incubation times. This novel Cys-S-SePy adduct is able to be chemoselectively reduced by five-fold excess ascorbate at pH 4.5, a condition that should spare already installed peptide disulfide bonds from reduction. This chemoselective reduction by ascorbate will undoubtedly find utility in numerous biotechnological applications. We applied our new chemistry to the iodine-free synthesis of the human intestinal hormone guanylin, which contains two disulfide bonds. While we originally envisioned using ascorbate to chemoselectively reduce one of the formed Cys-S-SePy adducts to catalyze disulfide bond formation, we found that when pairs of Cys(Acm) residues were treated with PySeSePy in TFA, the second disulfide bond formed spontaneously. Spontaneous formation of the second disulfide is most likely driven by the formation of the thermodynamically favored diselenide (PySeSePy) from the two Cys-S-SePy adducts. Thus, we have developed a one-pot method for concomitant deprotection and disulfide bond formation of Cys(Acm) pairs in the presence of an existing disulfide bond.