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. 2001 Sep 7;293(5536):1793-800.
doi: 10.1126/science.293.5536.1793.

Structure of MsbA from E. coli: a homolog of the multidrug resistance ATP binding cassette (ABC) transporters

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Structure of MsbA from E. coli: a homolog of the multidrug resistance ATP binding cassette (ABC) transporters

G Chang et al. Science. .

Retraction in

  • Retraction.
    Chang G, Roth CB, Reyes CL, Pornillos O, Chen YJ, Chen AP. Chang G, et al. Science. 2006 Dec 22;314(5807):1875. doi: 10.1126/science.314.5807.1875b. Science. 2006. PMID: 17185584 No abstract available.

Abstract

Multidrug resistance (MDR) is a serious medical problem and presents a major challenge to the treatment of disease and the development of novel therapeutics. ABC transporters that are associated with multidrug resistance (MDR-ABC transporters) translocate hydrophobic drugs and lipids from the inner to the outer leaflet of the cell membrane. To better elucidate the structural basis for the "flip-flop" mechanism of substrate movement across the lipid bilayer, we have determined the structure of the lipid flippase MsbA from Escherichia coli by x-ray crystallography to a resolution of 4.5 angstroms. MsbA is organized as a homodimer with each subunit containing six transmembrane alpha-helices and a nucleotide-binding domain. The asymmetric distribution of charged residues lining a central chamber suggests a general mechanism for the translocation of substrate by MsbA and other MDR-ABC transporters. The structure of MsbA can serve as a model for the MDR-ABC transporters that confer multidrug resistance to cancer cells and infectious microorganisms.

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