Literature DB >> 32633882

A Macrocyclic Peptide Library with a Structurally Constrained Cyclopropane-containing Building Block Leads to Thiol-independent Inhibitors of Phosphoglycerate Mutase.

Rika Okuma1, Tomoki Kuwahara2, Takafumi Yoshikane1, Mizuki Watanabe2, Patricia Dranchak3, James Inglese3, Satoshi Shuto2, Yuki Goto1, Hiroaki Suga1.   

Abstract

Here we report the construction of an mRNA-encoded library of thioether-closed macrocyclic peptides by using an N-chloroacetyl-cyclopropane-containing exotic initiator whose structure is more constrained than the ordinary N-chloroacetyl-α-amino acid initiators. The use of such an initiator has led to a macrocycle library with significantly suppressed population of lariat-shaped species compared with the conventional libraries. We previously used a conventional library and identified a small lariat thioether-macrocycle with a tail peptide with a C-terminal free Cys whose sidechain plays an essential role in potent inhibitory activity against a parasitic model enzyme, phosphoglycerate mutase. On the other hand, the cyclopropane-containing macrocycle library has yielded a larger thioether-macrocycle lacking a free Cys residue, which exhibits potent inhibitory activity to the same enzyme with a different mode of action. This result indicates that such a cyclopropane-containing macrocycle library would allow us to access mechanistically distinct macrocycles.
© 2020 Wiley-VCH Verlag GmbH & Co. KGaA, Weinheim.

Entities:  

Keywords:  cyclopropane; genetic code reprogramming; mRNA display; macrocyclic peptide

Mesh:

Substances:

Year:  2020        PMID: 32633882      PMCID: PMC9547493          DOI: 10.1002/asia.202000700

Source DB:  PubMed          Journal:  Chem Asian J        ISSN: 1861-471X


  52 in total

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4.  RNA-peptide fusions for the in vitro selection of peptides and proteins.

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5.  Cyclopropane-Based Peptidomimetics Mimicking Wide-Ranging Secondary Structures of Peptides: Conformational Analysis and Their Use in Rational Ligand Optimization.

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Journal:  Chemistry       Date:  2017-02-01       Impact factor: 5.236

6.  Three-dimensional structural diversity-oriented peptidomimetics based on the cyclopropylic strain.

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7.  Ribosomal Synthesis of Backbone-Cyclic Peptides Compatible with In Vitro Display.

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3.  Structure-activity relationship of ipglycermide binding to phosphoglycerate mutases.

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4.  Highly Efficient Cyclization Approach of Propargylated Peptides via Gold(I)-Mediated Sequential C-N, C-O, and C-C Bond Formation.

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