The Barbamide Biosynthetic Gene Cluster: a Novel Marine Cyanobacterial System of Mixed Polyketide Synthase (PKS)-non-ribosomal Peptide Synthetase (NRPS) Origin Involving an Unusual Trichloroleucyl Starter Unit

Overview

Journal Gene

Specialty Molecular Biology

Date 2002 Oct 18

PMID 12383521

Citations 76

Authors

Zunxue Chang

Patricia Flatt

William H Gerwick

Viet-Anh Nguyen

Christine L Willis

David H Sherman

Affiliations

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Abstract

Barbamide was extracted from the marine cyanobacterium Lyngbya majuscula strain 19L as a chlorinated lipopeptide for its potent molluscicidal activity. Precursor incorporation studies indicated that it is derived from acetate, L-phenylalanine, L-leucine and L-cysteine. The gene cluster responsible for biosynthesis of barbamide (bar) was cloned and characterized in this study. DNA sequence analysis of cosmid pLM49 revealed a cluster of 12 open reading frames (barA-barK) extending 26 kb including the expected polyketide synthase and non-ribosomal peptide synthetase modules and tailoring genes. The genetic architecture and domain organization of the bar cluster supports the assignment based on the apparent co-linearity of the systems. The activity assay of adenylation domains of barD (A(D)), barE (A(E)) and barG (A(G2) for module 2) in an amino acid-dependent ATP-pyrophosphate exchange experiment supports the conclusion that barbamide is synthesized from acetate, L-phenylalanine, L-cysteine and L-leucine with trichloroleucine as a direct precursor by a mixed polyketide synthase/non-ribosomal polypeptide synthetase. Assembly of barbamide includes unique biochemical mechanisms for chlorination, one-carbon truncation during chain elongation, E-double bond formation and thiazole ring formation.

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