Micrococcin cysteine-to-thiazole conversion through transient interactions between the scaffolding protein TclI and the modification enzymes TclJ and TclN.
Diana G Calvopina-ChavezDevan M BurseyYi-Jie TsengLeena M PatilKathryn D BewleyPhilip R BennallackJosh M McPhieKimberly B WagstaffAnisha DaleySusan M MillerJames D MoodyJohn C PriceJoel S GriffittsPublished in: Applied and environmental microbiology (2024)
Thiopeptides are a family of antimicrobial peptides characterized for having sulfur-containing heterocycles and for being highly post-translationally modified. Numerous thiopeptides have been identified; almost all of which inhibit protein synthesis in gram-positive bacteria. These intrinsic antimicrobial properties make thiopeptides promising candidates for the development of new antibiotics. The thiopeptide micrococcin is synthesized by the ribosome and undergoes several post-translational modifications to acquire its bioactivity. In this study, we identify key interactions within the enzymatic complex that carries out cysteine to thiazole conversion in the biosynthesis of micrococcin.