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Exploring the Mechanism of General Anesthesia: Kinetic Analysis of GABA(A) Receptor Electrophysiology

  • D. K. Lee
  • , D. J. Albershardt
  • , Robert S. Cantor
    • Dartmouth College

    Publikation: Bidrag til tidsskriftTidsskriftartikelForskningpeer review

    Abstract

    A kinetic model of the effect of agonist and anesthetics on ligand-gated ion channels, developed in earlier work, is further refined and used to predict traces observed in fast-perfusion electrophysiological studies on recombinant GABAA receptors under a wide range of agonist and/or anesthetic concentrations. The model incorporates only three conformational states (resting, open, and desensitized) but allows for the modulation of the conformational free energy landscape connecting these states resulting from adsorption of agonist and/or anesthetic to the bilayer in which the protein is embedded. The model is shown to reproduce the diverse and complex features of experimental traces remarkably well, including both anesthetic-induced and agonist-induced traces, as well as the modulation of agonist-induced traces by anesthetic, either coapplied or continuously present. The solutions to the kinetic equations, which give the time-dependence of each of the nine protein states (three ligation states for each of the three conformations), describe the flow of probability among these states and thus reveal the kinetic underpinnings of the traces. Many of the parameters in the model, such as the desorption rate constants of anesthetic and agonist, are directly related to model-independent experimental measurements and thus can serve as a definitive test of its validity.

    OriginalsprogEngelsk
    TidsskriftBiophysical Journal
    Vol/bind108
    Udgave nummer5
    Sider (fra-til)1081-1093
    ISSN0006-3495
    DOI
    StatusUdgivet - 2015

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