학술논문
The biosynthesis of methanobactin
Document Type
research-article
Author
Kenney, Grace E.; Dassama, Laura M. K.; Pandelia, Maria-Eirini; Gizzi, Anthony S.; Martinie, Ryan J.; Gao, Peng; DeHart, Caroline J.; Schachner, Luis F.; Skinner, Owen S.; Ro, Soo Y.; Zhu, Xiao; Sadek, Monica; Thomas, Paul M.; Almo, Steven C.; Bollinger, J. Martin; Krebs, Carsten; Kelleher, Neil L.; Rosenzweig, Amy C.
Source
Science, 2018 Mar . 359(6382), 1411-1416.
Subject
Language
English
ISSN
00368075
10959203
10959203
Abstract
Metal homeostasis poses a major challenge to microbes, which must acquire scarce elements for core metabolic processes. Methanobactin, an extensively modified copper-chelating peptide, was one of the earliest natural products shown to enable microbial acquisition of a metal other than iron. We describe the core biosynthetic machinery responsible for the characteristic posttranslational modifications that grant methanobactin its specificity and affinity for copper. A heterodimer comprising MbnB, a DUF692 family iron enzyme, and MbnC, a protein from a previously unknown family, performs a dioxygen-dependent four-electron oxidation of the precursor peptide (MbnA) to install an oxazolone and an adjacent thioamide, the characteristic methanobactin bidentate copper ligands. MbnB and MbnC homologs are encoded together and separately in many bacterial genomes, suggesting functions beyond their roles in methanobactin biosynthesis.