Interplay of Nav1.8 and Nav1.7 channels drives neuronal hyperexcitability in neuropathic pain.

IF 3.3 2区 医学 Q1 PHYSIOLOGY Journal of General Physiology Pub Date : 2024-11-04 Epub Date: 2024-10-08 DOI:10.1085/jgp.202413596
Dmytro V Vasylyev, Peng Zhao, Betsy R Schulman, Stephen G Waxman
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Abstract

While voltage-gated sodium channels Nav1.7 and Nav1.8 both contribute to electrogenesis in dorsal root ganglion (DRG) neurons, details of their interactions have remained unexplored. Here, we studied the functional contribution of Nav1.8 in DRG neurons using a dynamic clamp to express Nav1.7L848H, a gain-of-function Nav1.7 mutation that causes inherited erythromelalgia (IEM), a human genetic model of neuropathic pain, and demonstrate a profound functional interaction of Nav1.8 with Nav1.7 close to the threshold for AP generation. At the voltage threshold of -21.9 mV, we observed that Nav1.8 channel open-probability exceeded Nav1.7WT channel open-probability ninefold. Using a kinetic model of Nav1.8, we showed that a reduction of Nav1.8 current by even 25-50% increases rheobase and reduces firing probability in small DRG neurons expressing Nav1.7L848H. Nav1.8 subtraction also reduces the amplitudes of subthreshold membrane potential oscillations in these cells. Our results show that within DRG neurons that express peripheral sodium channel Nav1.7, the Nav1.8 channel amplifies excitability at a broad range of membrane voltages with a predominant effect close to the AP voltage threshold, while Nav1.7 plays a major role at voltages closer to resting membrane potential. Our data show that dynamic-clamp reduction of Nav1.8 conductance by 25-50% can reverse hyperexcitability of DRG neurons expressing a gain-of-function Nav1.7 mutation that causes pain in humans and suggests, more generally, that full inhibition of Nav1.8 may not be required for relief of pain due to DRG neuron hyperexcitability.

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Nav1.8和Nav1.7通道的相互作用驱动了神经元在神经病理性疼痛中的过度兴奋。
虽然电压门控钠通道 Nav1.7 和 Nav1.8 都有助于背根神经节(DRG)神经元的电发生,但它们之间相互作用的细节仍未得到探索。在这里,我们使用动态钳夹表达 Nav1.7L848H(一种导致遗传性红斑性神经痛(IEM)的功能增益型 Nav1.7 突变),研究了 Nav1.8 在 DRG 神经元中的功能贡献,并证明了 Nav1.8 与 Nav1.7 在接近 AP 生成阈值时的深刻功能相互作用。在 -21.9 mV 的电压阈值,我们观察到 Nav1.8 通道的开放概率是 Nav1.7WT 通道开放概率的九倍。通过使用 Nav1.8 的动力学模型,我们发现在表达 Nav1.7L848H 的小 DRG 神经元中,Nav1.8 电流即使减少 25-50%,也会增加流变基数并降低点火概率。在这些细胞中,Nav1.8 减弱也会降低阈下膜电位振荡的振幅。我们的研究结果表明,在表达外周钠通道 Nav1.7 的 DRG 神经元中,Nav1.8 通道在很宽的膜电压范围内放大兴奋性,在接近 AP 电压阈值时起主要作用,而 Nav1.7 在接近静息膜电位时起主要作用。我们的数据表明,动态钳夹将 Nav1.8 的电导降低 25-50% 可以逆转表达 Nav1.7 功能增益突变的 DRG 神经元的过度兴奋性,而这种突变会导致人类疼痛。
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来源期刊
CiteScore
6.00
自引率
10.50%
发文量
88
审稿时长
6-12 weeks
期刊介绍: General physiology is the study of biological mechanisms through analytical investigations, which decipher the molecular and cellular mechanisms underlying biological function at all levels of organization. The mission of Journal of General Physiology (JGP) is to publish mechanistic and quantitative molecular and cellular physiology of the highest quality, to provide a best-in-class author experience, and to nurture future generations of independent researchers. The major emphasis is on physiological problems at the cellular and molecular level.
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