4.3 Article

Local Anesthetics Disrupt Energetic Coupling between the Voltage-sensing Segments of a Sodium Channel

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JOURNAL OF GENERAL PHYSIOLOGY
卷 133, 期 1, 页码 1-15

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ROCKEFELLER UNIV PRESS
DOI: 10.1085/jgp.200810103

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资金

  1. National Institutes of Health [GM084140-01]
  2. AHA [0535214N]
  3. Shaw Scientist award
  4. NATIONAL INSTITUTE OF GENERAL MEDICAL SCIENCES [R01GM084140] Funding Source: NIH RePORTER

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Local anesthetics block sodium channels in a state-dependent fashion, binding with higher affinity to open and/or inactivated states. Gating current measurements show that local anesthetics immobilize a fraction of the gating charge, suggesting that the movement of voltage sensors is modified when a local anesthetic binds to the pore of the sodium channel. Here, using voltage clamp fluorescence measurements, we provide a quantitative description of the effect of local anesthetics on the steady-state behavior of the voltage-sensing segments of a sodium channel. Lidocaine and QX-314 shifted the midpoints of the fluorescence-voltage (F-V) curves of S4 domain III in the hyperpolarizing direction by 57 and 65 mV, respectively. A single mutation in the S6 of domain IV (F1579A), a site critical for local anesthetic block, abolished the effect of QX-314 on the voltage sensor of domain III. Both local anesthetics modestly shifted the F-V relationships of S4 domain IV toward hyperpolarized potentials. In contrast, the F-V curve of the S4 domain I was shifted by 11 mV in the depolarizing direction upon QX-314 binding. These antagonistic effects of the local anesthetic indicate that the drug modifies the coupling between the voltage-sensing domains of the sodium channel. Our findings suggest a novel role of local anesthetics in modulating the gating apparatus of the sodium channel.

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