Abstract
The progress of total chemical protein synthesis has been hampered by difficulties in preparing peptide thioesters by standard Fmoc peptide synthesis. The amino acid, α-methylcysteine, sited at the C-terminus of a peptide can substitute for a thioester in peptide ligation reactions. C-terminal α-methylcysteine is fully compatible with Fmoc peptide synthesis and its use in ligation is very simple and robust. Its potential is demonstrated with the synthesis of model proteins. © 2014 The Royal Society of Chemistry.
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CITATION STYLE
Burlina, F., Papageorgiou, G., Morris, C., White, P. D., & Offer, J. (2013). In situ thioester formation for protein ligation using α-methylcysteine. Chemical Science, 5(2), 766–770. https://doi.org/10.1039/c3sc52140k
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