TRPV1 通道在慢性间歇性缺氧后对孤束核中自发谷氨酸释放有贡献。
TRPV1 channels contribute to spontaneous glutamate release in nucleus tractus solitarii following chronic intermittent hypoxia.
机构信息
Department of Biomedical Sciences, University of Missouri , Columbia, Missouri.
Dalton Cardiovascular Research Center, University of Missouri , Columbia, Missouri.
出版信息
J Neurophysiol. 2019 Mar 1;121(3):881-892. doi: 10.1152/jn.00536.2018. Epub 2019 Jan 2.
Chronic intermittent hypoxia (CIH) reduces afferent-evoked excitatory postsynaptic currents (EPSCs) but enhances basal spontaneous (s) and asynchronous (a) EPSCs in second-order neurons of nucleus tractus solitarii (nTS), a major area for cardiorespiratory control. The net result is an increase in synaptic transmission. The mechanisms by which this occurs are unknown. The N-type calcium channel and transient receptor potential cation channel TRPV1 play prominent roles in nTS sEPSCs and aEPSCs. The functional role of these channels in CIH-mediated afferent-evoked EPSC, sEPSC, and aEPSC was tested in rat nTS slices following antagonist inhibition and in mouse nTS slices that lack TRPV1. Block of N-type channels decreased aEPSCs in normoxic and, to a lesser extent, CIH-exposed rats. sEPSCs examined in the presence of TTX (miniature EPSCs) were also decreased by N-type block in normoxic but not CIH-exposed rats. Antagonist inhibition of TRPV1 reduced the normoxic and the CIH-mediated increase in sEPSCs, aEPSCs, and mEPSCs. As in rats, in TRPV1 control mice, aEPSCs, sEPSCs, and mEPSCs were enhanced following CIH. However, none were enhanced in TRPV1 null mice. Normoxic tractus solitarii (TS)-evoked EPSC amplitude, and the decrease after CIH, were comparable in control and null mice. In rats, TRPV1 was localized in the nodose-petrosal ganglia (NPG) and their central branches. CIH did not alter TRPV1 mRNA but increased its protein in NPG consistent with an increased contribution of TRPV1. Together, our studies indicate TRPV1 contributes to the CIH increase in aEPSCs and mEPSCs, but the CIH reduction in TS-EPSC amplitude occurs via an alternative mechanism. NEW & NOTEWORTHY This study provides information on the underlying mechanisms responsible for the chronic intermittent hypoxia (CIH) increase in synaptic transmission that leads to exaggerated sympathetic nervous and respiratory activity at baseline and in response to low oxygen. We demonstrate that the CIH increase in asynchronous and spontaneous excitatory postsynaptic currents (EPSCs) and miniature EPSCs, but not decrease in afferent-driven EPSCs, is dependent on transient receptor potential vanilloid type 1 (TRPV1). Thus TRPV1 is important in controlling nucleus tractus solitarii synaptic activity during CIH.
慢性间歇性低氧(CIH)会降低传入诱发的兴奋性突触后电流(EPSC),但会增强孤束核(nTS)中第二级神经元的基础自发性(s)和异步(a)EPSC,nTS 是心肺控制的主要区域。净结果是突触传递增加。其发生的机制尚不清楚。N 型钙通道和瞬时受体电位阳离子通道 TRPV1 在 nTS 的 sEPSC 和 aEPSC 中起重要作用。在使用拮抗剂抑制以及在缺乏 TRPV1 的小鼠 nTS 切片中,测试了这些通道在 CIH 介导的传入诱发 EPSC、sEPSC 和 aEPSC 中的功能作用。在正常氧合和更轻微的 CIH 暴露的大鼠中,N 型通道阻断减少了 aEPSC。在正常氧合但不在 CIH 暴露的大鼠中,TTX 存在时检查的 sEPSC(微小 EPSC)也被 N 型阻断减少。TRPV1 拮抗剂抑制降低了正常氧合和 CIH 介导的 sEPSC、aEPSC 和 mEPSC 的增加。与大鼠一样,在 TRPV1 对照小鼠中,CIH 后 aEPSC、sEPSC 和 mEPSC 增强。然而,在 TRPV1 缺失的小鼠中,它们均未增强。正常氧合孤束核(TS)诱发的 EPSC 幅度以及 CIH 后的减少在对照和缺失小鼠中是可比的。在大鼠中,TRPV1 位于结状神经节(NPG)及其中央分支中。CIH 没有改变 NPG 中的 TRPV1 mRNA,但增加了其蛋白,这与 TRPV1 的贡献增加一致。总的来说,我们的研究表明 TRPV1 有助于 CIH 增加 aEPSC 和 mEPSC,但 TS-EPSC 幅度的 CIH 减少是通过另一种机制发生的。本研究提供了有关导致基础交感神经和呼吸活动在基线和低氧反应时过度增加的慢性间歇性低氧(CIH)增加突触传递的潜在机制的信息。我们证明,CIH 增加异步和自发性兴奋性突触后电流(EPSC)和微小 EPSC,但传入驱动的 EPSC 减少,这取决于瞬时受体电位香草醛 1 型(TRPV1)。因此,TRPV1 在 CIH 期间控制孤束核突触活动中很重要。
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