| Literature DB >> 29215779 |
Jian Gao1, Tzu-Ping Ko2, Lu Chen3, Satish R Malwal4, Jianan Zhang5, Xiangying Hu1, Fiona Qu4, Weidong Liu1, Jian-Wen Huang1, Ya-Shan Cheng1, Chun-Chi Chen1, Yunyun Yang6, Yonghui Zhang6, Eric Oldfield4,7, Rey-Ting Guo1.
Abstract
We report the first X-ray crystallographic structure of the "head-to-middle" prenyltransferase, isosesquilavandulyl diphosphate synthase, involved in biosynthesis of the merochlorin class of antibiotics. The protein adopts the ζ or cis-prenyl transferase fold but remarkably, unlike tuberculosinol adenosine synthase and other cis-prenyl transferases (e.g. cis-farnesyl, decaprenyl, undecaprenyl diphosphate synthases), the large, hydrophobic side chain does not occupy a central hydrophobic tunnel. Instead, it occupies a surface pocket oriented at 90° to the hydrophobic tunnel. Product chain-length control is achieved by squeezing out the ligand from the conventional allylic S1 binding site, with proton abstraction being achieved using a diphosphate-Asn-Ser relay. The structures revise and unify our thinking as to the mechanism of action of many other prenyl transferases and may also be of use in engineering new merochlorin-class antibiotics.Entities:
Keywords: X-ray diffraction; antibiotics; enzymes; isoprenoids; protein structures
Year: 2017 PMID: 29215779 DOI: 10.1002/anie.201710185
Source DB: PubMed Journal: Angew Chem Int Ed Engl ISSN: 1433-7851 Impact factor: 15.336