Structure and lipid dynamics in the maintenance of lipid asymmetry inner membrane complex of A. baumannii

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作者
Daniel Mann
Junping Fan
Kamolrat Somboon
Daniel P. Farrell
Andrew Muenks
Svetomir B. Tzokov
Frank DiMaio
Syma Khalid
Samuel I. Miller
Julien R. C. Bergeron
机构
[1] The University of Sheffield,Department of Molecular Biology and Biotechnology
[2] The University of Washington,Department of Microbiology
[3] University of Southampton,Department of Chemistry
[4] The University of Washington,Department of Biochemistry
[5] The University of Washington,Department of Genetics
[6] The University of Washington,Department of Medicine
[7] King’s College London,Randall Division of Cell and Molecular Biophysics
[8] Ernst-Ruska-Centre 3,Department of Chemical Biology
[9] Peking University,undefined
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Multi-resistant bacteria are a major threat in modern medicine. The gram-negative coccobacillus Acinetobacter baumannii currently leads the WHO list of pathogens in critical need for new therapeutic development. The maintenance of lipid asymmetry (MLA) protein complex is one of the core machineries that transport lipids from/to the outer membrane in gram-negative bacteria. It also contributes to broad-range antibiotic resistance in several pathogens, most prominently in A. baumannii. Nonetheless, the molecular details of its role in lipid transport has remained largely elusive. Here, we report the cryo-EM maps of the core MLA complex, MlaBDEF, from the pathogen A. baumannii, in the apo-, ATP- and ADP-bound states, revealing multiple lipid binding sites in the cytosolic and periplasmic side of the complex. Molecular dynamics simulations suggest their potential trajectory across the membrane. Collectively with the recently-reported structures of the E. coli orthologue, this data also allows us to propose a molecular mechanism of lipid transport by the MLA system.
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