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双酚 A 对小鼠背根神经节神经元电压门控钠通道的抑制作用。

Inhibition of voltage-gated sodium channels by bisphenol A in mouse dorsal root ganglion neurons.

机构信息

Department of Toxicology, School of Public Health, Nanjing Medical University, 140 Hanzhong Road, Nanjing 210029, China.

出版信息

Brain Res. 2011 Mar 10;1378:1-8. doi: 10.1016/j.brainres.2011.01.022. Epub 2011 Jan 15.

Abstract

Bisphenol A (BPA), an estrogenic compound, is contained in cans, polycarbonate bottles, and some dental sealants. Exposure to BPA might have potential toxicological effects on the nervous system. Previous studies have demonstrated that BPA may affect ion channel function, but the effects of BPA on voltage-gated sodium channels are unknown. Herein, we report the effects of BPA on TTX-sensitive (TTX-S) and TTX-resistant (TTX-R) Na+ currents, using a conventional whole-cell patch clamp technique from acutely isolated mouse dorsal root ganglion neurons. BPA inhibited TTX-S Na+ currents and TTX-R Na+ currents, the effects of BPA were rapid, reversible and in a concentration-dependent manner. Moreover, BPA could shift the voltage-gated activation curve for TTX-S Na+ channel in the hyperpolarizing direction without changing that for TTX-R Na+ channel; shift the steady-state inactivation curve for TTX-S Na+ channel in the depolarizing direction without changing that for TTX-R Na+ channel; and lengthen the time course of recovery from inactivation for both TTX-S Na+ current and TTX-R Na+ current. We also found that PKC inhibitor GÖ-6983 and PKA inhibitor H-89 blocked the BPA-induced inhibition of Na+ currents. Considering its complex modulatory effects on voltage-gated sodium channels, BPA might have potential toxicological effects on the nervous system and lead to a change in excitability of nociceptive afferent fibers.

摘要

双酚 A(BPA)是一种雌激素化合物,存在于罐头、聚碳酸酯瓶和一些牙科密封剂中。接触 BPA 可能对神经系统产生潜在的毒理学影响。先前的研究表明,BPA 可能影响离子通道功能,但 BPA 对电压门控钠通道的影响尚不清楚。在此,我们使用从急性分离的小鼠背根神经节神经元中获得的常规全细胞膜片钳技术,报告了 BPA 对 TTX 敏感(TTX-S)和 TTX 抗性(TTX-R)Na+电流的影响。BPA 抑制 TTX-S Na+电流和 TTX-R Na+电流,BPA 的作用迅速、可逆且呈浓度依赖性。此外,BPA 可以将 TTX-S Na+通道的电压门控激活曲线向超极化方向移动,而不改变 TTX-R Na+通道的激活曲线;将 TTX-S Na+通道的稳态失活曲线向去极化方向移动,而不改变 TTX-R Na+通道的失活曲线;并延长 TTX-S Na+电流和 TTX-R Na+电流的失活后恢复时间过程。我们还发现 PKC 抑制剂 GÖ-6983 和 PKA 抑制剂 H-89 阻断了 BPA 诱导的 Na+电流抑制。考虑到 BPA 对电压门控钠通道的复杂调节作用,BPA 可能对神经系统产生潜在的毒理学影响,并导致伤害性传入纤维兴奋性的变化。

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