| Literature DB >> 29720648 |
Hoangdung Ho1, Anh Miu2, Mary Kate Alexander3, Natalie K Garcia4, Angela Oh1, Inna Zilberleyb5, Mike Reichelt6, Cary D Austin6, Christine Tam5, Stephanie Shriver5, Huiyong Hu7, Sharada S Labadie7, Jun Liang7, Lan Wang7, Jian Wang8, Yan Lu8, Hans E Purkey7, John Quinn2, Yvonne Franke5, Kevin Clark2, Maureen H Beresini2, Man-Wah Tan3, Benjamin D Sellers7, Till Maurer1, Michael F T Koehler7, Aaron T Wecksler4, James R Kiefer1, Vishal Verma7, Yiming Xu2, Mireille Nishiyama3, Jian Payandeh9,10, Christopher M Koth11,12.
Abstract
The movement of core-lipopolysaccharide across the inner membrane of Gram-negative bacteria is catalysed by an essential ATP-binding cassette transporter, MsbA. Recent structures of MsbA and related transporters have provided insights into the molecular basis of active lipid transport; however, structural information about their pharmacological modulation remains limited. Here we report the 2.9 Å resolution structure of MsbA in complex with G907, a selective small-molecule antagonist with bactericidal activity, revealing an unprecedented mechanism of ABC transporter inhibition. G907 traps MsbA in an inward-facing, lipopolysaccharide-bound conformation by wedging into an architecturally conserved transmembrane pocket. A second allosteric mechanism of antagonism occurs through structural and functional uncoupling of the nucleotide-binding domains. This study establishes a framework for the selective modulation of ABC transporters and provides rational avenues for the design of new antibiotics and other therapeutics targeting this protein family.Entities:
Mesh:
Substances:
Year: 2018 PMID: 29720648 DOI: 10.1038/s41586-018-0083-5
Source DB: PubMed Journal: Nature ISSN: 0028-0836 Impact factor: 49.962