Literature DB >> 18570870

The mechanism of a neurotransmitter:sodium symporter--inward release of Na+ and substrate is triggered by substrate in a second binding site.

Lei Shi1, Matthias Quick, Yongfang Zhao, Harel Weinstein, Jonathan A Javitch.   

Abstract

Eukaryotic neurotransmitter:sodium symporters (NSSs), targets for antidepressants and psychostimulants, terminate neurotransmission by sodium-driven reuptake. The crystal structure of LeuT(Aa), a prokaryotic NSS homolog, revealed an occluded state in which one leucine and two Na(+) ions are bound, but provided limited clues to the molecular mechanism of transport. Using steered molecular dynamics simulations, we explored the substrate translocation pathway of LeuT. We identified a second substrate binding site located in the extracellular vestibule comprised of residues shown recently to participate in binding tricyclic antidepressants. Binding and flux experiments showed that the two binding sites can be occupied simultaneously. The substrate in the secondary site allosterically triggers intracellular release of Na(+) and substrate from the primary site, thereby functioning as a "symport effector." Because tricyclic antidepressants bind differently to this secondary site, they do not promote substrate release from the primary site and thus act as symport uncouplers and inhibit transport.

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Year:  2008        PMID: 18570870      PMCID: PMC2826427          DOI: 10.1016/j.molcel.2008.05.008

Source DB:  PubMed          Journal:  Mol Cell        ISSN: 1097-2765            Impact factor:   17.970


  35 in total

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8.  An intracellular interaction network regulates conformational transitions in the dopamine transporter.

Authors:  Julie Kniazeff; Lei Shi; Claus J Loland; Jonathan A Javitch; Harel Weinstein; Ulrik Gether
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  221 in total

1.  Identification of a second substrate-binding site in solute-sodium symporters.

Authors:  Zheng Li; Ashley S E Lee; Susanne Bracher; Heinrich Jung; Aviv Paz; Jay P Kumar; Jeff Abramson; Matthias Quick; Lei Shi
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2.  Simulations of the alternating access mechanism of the sodium symporter Mhp1.

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3.  It takes two to transport, or is it one?

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Review 4.  The solute carrier 6 family of transporters.

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5.  Quantitative modeling of membrane deformations by multihelical membrane proteins: application to G-protein coupled receptors.

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6.  Insights into transport mechanism from LeuT engineered to transport tryptophan.

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8.  Conformational rearrangements to the intracellular open states of the LeuT and ApcT transporters are modulated by common mechanisms.

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9.  Substrate-induced unlocking of the inner gate determines the catalytic efficiency of a neurotransmitter:sodium symporter.

Authors:  Christian B Billesbølle; Mie B Krüger; Lei Shi; Matthias Quick; Zheng Li; Sebastian Stolzenberg; Julie Kniazeff; Kamil Gotfryd; Jonas S Mortensen; Jonathan A Javitch; Harel Weinstein; Claus J Loland; Ulrik Gether
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10.  A competitive inhibitor traps LeuT in an open-to-out conformation.

Authors:  Satinder K Singh; Chayne L Piscitelli; Atsuko Yamashita; Eric Gouaux
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