Functionally-selective inhibition of threshold sodium currents and excitability in dorsal root ganglion neurons by cannabinol

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作者
Mohammad-Reza Ghovanloo
Philip R. Effraim
Sidharth Tyagi
Peng Zhao
Sulayman D. Dib-Hajj
Stephen G. Waxman
机构
[1] Yale University School of Medicine,Department of Neurology
[2] Yale University,Center for Neuroscience & Regeneration Research
[3] Neuro-Rehabilitation Research Center,Department of Anesthesiology
[4] Veterans Affairs Connecticut Healthcare System,Medical Scientist Training Program
[5] Yale University School of Medicine,undefined
[6] Yale University School of Medicine,undefined
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Communications Biology | / 7卷
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摘要
Cannabinol (CBN), an incompletely understood metabolite for ∆9-tetrahydrocannabinol, has been suggested as an analgesic. CBN interacts with endocannabinoid (CB) receptors, but is also reported to interact with non-CB targets, including various ion channels. We assessed CBN effects on voltage-dependent sodium (Nav) channels expressed heterologously and in native dorsal root ganglion (DRG) neurons. Our results indicate that CBN is a functionally-selective, but structurally-non-selective Nav current inhibitor. CBN’s main effect is on slow inactivation. CBN slows recovery from slow-inactivated states, and hyperpolarizes steady-state inactivation, as channels enter deeper and slower inactivated states. Multielectrode array recordings indicate that CBN attenuates DRG neuron excitability. Voltage- and current-clamp analysis of freshly isolated DRG neurons via our automated patch-clamp platform confirmed these findings. The inhibitory effects of CBN on Nav currents and on DRG neuron excitability add a new dimension to its actions and suggest that this cannabinoid may be useful for neuropathic pain.
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