Reassignment of the Structure of a Tryptophan‐Containing Cyclic Tripeptide Produced by the Biarylitide Crosslinking Cytochrome P450blt

Author:

Coe Laura J.1,Zhao Yongwei234,Padva Leo5,Keto Angus1,Schittenhelm Ralf6,Tailhades Julien234,Pierens Greg7,Krenske Elizabeth H.1,Crüsemann Max5,De Voss James J.14,Cryle Max J.234ORCID

Affiliation:

1. School of Chemistry and Molecular Biosciences The University of Queensland Brisbane QLD 4072 Australia

2. Department of Biochemistry and Molecular Biology The Monash Biomedicine Discovery Institute Monash University Clayton VIC 3800 Australia

3. EMBL Australia Monash University Clayton VIC 3800 Australia

4. ARC Centre of Excellence for Innovations in Peptide and Protein Science Australia

5. Institute of Pharmaceutical Biology University of Bonn 53115 Bonn Germany

6. Monash Proteomics and Metabolomics Platform Monash University Clayton VIC 3800 Australia

7. Centre for Advanced Imaging The University of Queensland Brisbane QLD 4072 Australia

Abstract

AbstractThe structure of the sidechain crosslinked Tyr‐Leu‐Trp peptide produced by the biarylitide crosslinking cytochrome P450Blt from Micromonospora sp. MW‐13 has been reanalysed by a series of NMR, computational and isotope labelling experiments and shown to contain a C−N rather than a C−O bond. Additional in vivo experiments using such a modified peptide show there is a general tolerance of biarylitide crosslinking P450 enzymes for histidine to tryptophan mutations within their minimal peptide substrate sequences despite the lack of such residues noted in natural biarylitide gene clusters. This work further highlights the impressive ability of P450s from biarylitide biosynthesis pathways to act as biocatalysts for the formation of a range of sidechain crosslinked tripeptides.

Funder

Australian Research Council

Publisher

Wiley

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