Biocompatible and selective generation of bicyclic peptides

06 June 2022, Version 1
This content is a preprint and has not undergone peer review at the time of posting.

Abstract

Bicyclic peptides possess superior properties for drug discovery; however, their chemical synthesis is not straightforward and often neither biocompatible nor fully orthogonal to all canonical amino acids. The selective reaction between 1,2-aminothiols and 2,6-dicyanopyridine allows direct access to complex bicyclic peptides in high yield. The process can be fully automated using standard solid-phase peptide synthesis. Bicyclization occurs in water at physiological pH within minutes and without the need for a catalyst. The use of various linkers allows tailored bicyclic peptides with qualities such as plasma stability, conformational preorganization, and high target affinity. We demonstrate this for a bicyclic inhibitor of the Zika virus protease NS2B-NS3 as well as for bicyclic versions of the α-helical antimicrobial peptide aurein 1.2.

Keywords

Peptides
Bicycles
Aminothiol-nitrile reaction
Macrocyclization
Cyanopyridine

Supplementary materials

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Supplementary figures, schemes and tables. Full description of experiments and compound characterisation.
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