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Structural basis for precursor protein-directed ribosomal peptide macrocyclization.

Nat. Chem. Biol.. 2016-03; 
LiKunhua,CondursoHeather L,LiGengnan,DingYousong,BrunerStev
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Gene Synthesis Full-length MdnA (residues1–49) (Genscript, USA and SynPeptide), MdnA1–35 (SynPeptide), MdnA11–49 (LifeTein) and MdnAAc20–49 (EZBioLabs) were purchased from custom peptide suppliers. Get A Quote

摘要

Macrocyclization is a common feature of natural product biosynthetic pathways including the diverse family of ribosomal peptides. Microviridins are architecturally complex cyanobacterial ribosomal peptides that target proteases with potent reversible inhibition. The product structure is constructed via three macrocyclizations catalyzed sequentially by two members of the ATP-grasp family, a unique strategy for ribosomal peptide macrocyclization. Here we describe in detail the structural basis for the enzyme-catalyzed macrocyclizations in the microviridin J pathway of Microcystis aeruginosa. The macrocyclases MdnC and MdnB interact with a conserved α-helix of the precursor peptide using a novel precursor-pepti... More

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