Affiliation:
1. Institute of Biomedical Sciences and Graduate School of Pharmaceutical Sciences Tokushima University Tokushima 770-8505 Japan
2. Faculty of Pharmacy and Pharmaceutical Sciences Fukuyama University Hiroshima 729-0292 Japan
3. Department of Diabetes Endocrinology and Nutrition Graduate School of Medicine Kyoto University Kyoto 606-8507 Japan
Abstract
AbstractA tyrosine (Tyr)‐ or tryptophan (Trp)‐selective metal‐free C−H sulfenylation reaction using an acid‐activated S‐acetamidomethyl cysteine (Cys) sulfoxide, Cys(Acm)(O), has been achieved. The dually protonated intermediate produced from Cys(Acm)(O) under acidic conditions allows the sulfenylation of Tyr. Significantly, the reaction in the presence of trimethylsilyl trifluoromethanesulfonate (TMSOTf) mainly affords a Cys‐Tyr‐linked peptide even in the presence of Trp residues. In contrast, a Cys‐Trp‐linked peptide was selectively obtained from the reaction in the presence of guanidine hydrochloride (Gn ⋅ HCl) under acidic conditions. Established Tyr‐ and Trp‐selective sulfenylation methods were used in the Cys‐Tyr stapling and Trp lipidation of glucagon‐like peptides 1 in a one‐pot/stepwise manner. Investigation of the mechanism showed that orbital‐ and charge‐controlled reactions are responsible for the Trp and Tyr selectivity, respectively.
Funder
Japan Agency for Medical Research and Development
Japan Society for the Promotion of Science
Subject
General Chemistry,Catalysis,Organic Chemistry
Cited by
6 articles.
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