Structural basis for dual-mode inhibition of the ABC transporter MsbA

被引:0
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作者
Hoangdung Ho
Anh Miu
Mary Kate Alexander
Natalie K. Garcia
Angela Oh
Inna Zilberleyb
Mike Reichelt
Cary D. Austin
Christine Tam
Stephanie Shriver
Huiyong Hu
Sharada S. Labadie
Jun Liang
Lan Wang
Jian Wang
Yan Lu
Hans E. Purkey
John Quinn
Yvonne Franke
Kevin Clark
Maureen H. Beresini
Man-Wah Tan
Benjamin D. Sellers
Till Maurer
Michael F. T. Koehler
Aaron T. Wecksler
James R. Kiefer
Vishal Verma
Yiming Xu
Mireille Nishiyama
Jian Payandeh
Christopher M. Koth
机构
[1] Genentech Inc.,Structural Biology
[2] Genentech Inc.,Biochemical and Cellular Pharmacology
[3] Genentech Inc.,Infectious Diseases
[4] Genentech Inc.,Protein Analytical Chemistry
[5] Genentech Inc.,Biomolecular Resources
[6] Genentech Inc.,Pathology
[7] Genentech Inc.,Discovery Chemistry
[8] WuXi Apptec. Co. Ltd.,undefined
来源
Nature | 2018年 / 557卷
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摘要
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.
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页码:196 / 201
页数:5
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