Peptide Modification via N‑Terminal-Residue-Directed γ‑C(sp3)−H Arylation

Zhen Lin Hou; Feipeng Yuan; Bo Yao

doi:10.1021/acs.orglett.0c03279

Peptide Modification via N‑Terminal-Residue-Directed γ‑C(sp³)−H Arylation

Zhen Lin Hou, Feipeng Yuan, Bo Yao^*

^*Corresponding author for this work

School of Chemistry and Chemical Engineering

Research output: Contribution to journal › Article › peer-review

15 Citations (Scopus)

Abstract

Postassembly modification of peptides via C(sp³)−H functionalization provides an efficient way to prepare functionalized peptides for biological study and pharmaceutical development. In this work, we developed a new method for γ-C(sp³)−H functionalization of aliphatic side chains of N-terminus-unprotected peptides. With the N-terminal residues as directing groups, a wide range of di-, tri-, tetra-, and pentapeptides underwent C−H arylation of the residues (Val, Ile, Tle) at the +2 position from the N-terminus.

Original language	English
Pages (from-to)	8692-8696
Number of pages	5
Journal	Organic Letters
Volume	22
Issue number	21
DOIs	https://doi.org/10.1021/acs.orglett.0c03279
Publication status	Published - 6 Nov 2020

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abstract = "Postassembly modification of peptides via C(sp3)−H functionalization provides an efficient way to prepare functionalized peptides for biological study and pharmaceutical development. In this work, we developed a new method for γ-C(sp3)−H functionalization of aliphatic side chains of N-terminus-unprotected peptides. With the N-terminal residues as directing groups, a wide range of di-, tri-, tetra-, and pentapeptides underwent C−H arylation of the residues (Val, Ile, Tle) at the +2 position from the N-terminus.",

author = "Hou, {Zhen Lin} and Feipeng Yuan and Bo Yao",

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AU - Hou, Zhen Lin

AU - Yuan, Feipeng

AU - Yao, Bo

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Y1 - 2020/11/6

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AB - Postassembly modification of peptides via C(sp3)−H functionalization provides an efficient way to prepare functionalized peptides for biological study and pharmaceutical development. In this work, we developed a new method for γ-C(sp3)−H functionalization of aliphatic side chains of N-terminus-unprotected peptides. With the N-terminal residues as directing groups, a wide range of di-, tri-, tetra-, and pentapeptides underwent C−H arylation of the residues (Val, Ile, Tle) at the +2 position from the N-terminus.

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Peptide Modification via N‑Terminal-Residue-Directed γ‑C(sp³)−H Arylation

Abstract

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