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    Biochemistry. 2008 Aug 5;47(31):7980-2. Epub 2008 Jul 11.

    Role of sequence bias in the topology of the multidrug transporter EmrE.

    McHaourab HS, Mishra S, Koteiche HA, Amadi SH.

    Department of Molecular Physiology and Biophysics, Vanderbilt University, Nashville, Tennessee 37232-0615, USA. hassane.mchaourab@vanderbilt.edu

    EmrE is the prototype of small multidrug resistance transporters and has emerged as a model of membrane protein evolution. Analysis of the distances separating symmetry-related site-specific spin labels, correlation of topological sequence bias to C-terminal orientation, to membrane insertion efficiency, and to resistance to ethidium bromide collectively demonstrate that EmrE monomers adopt a parallel topology in the functional dimer. We propose a coupled insertion and assembly model for EmrE in which the favorable energetics of the parallel dimer interface override topological constraints arising from weak asymmetry in positive charge distribution.

    PMID: 18616286 [PubMed - indexed for MEDLINE]

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