Chemoselective and photocleavable cysteine modification of peptides and proteins using isoxazoliniums

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作者
Jie-Ren Deng
Sai-Fung Chung
Alan Siu-Lun Leung
Wai-Ming Yip
Bin Yang
Man-Chung Choi
Jian-Fang Cui
Karen Ka-Yan Kung
Zhen Zhang
Kar-Wai Lo
Yun-Chung Leung
Man-Kin Wong
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[1] The Hong Kong Polytechnic University,State Key Laboratory of Chemical Biology and Drug Discovery, and Department of Applied Biology and Chemical Technology
[2] The Hong Kong Polytechnic University,Henry Cheng Research Laboratory for Drug Development and Lo Ka Chung Centre for Natural Anti
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It is of ongoing interest to develop new approaches for efficient and selective modification of cysteine residues on biomolecules. Here we present a comprehensive study on a newly developed isoxazolinium-mediated cysteine modification of peptides and proteins. Using a stoichiometric amount of isoxazolinium reagents generated in situ from a catalytic amount of silver salts, cysteine-containing peptides can be efficiently modified to afford products in nearly complete conversions. With the optimized conditions, free cysteine containing proteins HSA and BSA, as well as a site-directed mutated therapeutic protein (BCArg) can be efficiently and selectively labelled using small amounts of the isoxazolinium reagents. We find that the phenylacyl thioether linkage bearing an alkyne moiety can be rapidly cleaved under irradiation of UV-A light, giving the formation of a thioaldehyde moiety, which can be converted back to cysteine by reduction.
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