Incorporation of electrically charged N-alkyl amino acids into ribosomally synthesized peptides via post-translational conversion?
Chemical Science Pub Date: 2013-11-28 DOI: 10.1039/C3SC52744A
Abstract
N-Alkyl amino acids are invaluable building blocks for ribosomally synthesized peptides because they can increase proteolytic stability and cell-permeability of peptides. However, previous studies showed that N-alkyl amino acids bearing an electrically charged side-chain cannot be directly incorporated into ribosomally synthesized peptides. Here we report a simple and robust method for ribosomal synthesis of peptides containing charged N-alkyl amino acids. In this method, an N-alkyl amino acid precursor, in which the charge of the translation-incompatible charged N-alkyl amino acid is masked, is ribosomally incorporated into a peptide. Subsequently, the precursor is post-translationally converted into a charged N-alkyl amino acid by bio-orthogonal chemical or enzymatic reaction. Using this method, we demonstrate the efficient incorporation of amine- or carboxylate-containing N-alkyl amino acids into ribosomally synthesized peptides and its compatibility with our recently developed in vitro transcription–translation coupled with association of puromycin-linker (TRAP) display. This study represents an important step toward in vitro display selection from structurally diverse N-alkyl-peptide libraries that will facilitate the discovery of proteolytically stable and cell-permeable peptidomimetics from libraries with high diversity.
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Journal Name:Chemical Science
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CAS no.: 89640-58-4