Kopp-Scheinpflug Cornelia, Pigott Beatrice M, Forsythe Ian D
Division of Neurobiology, Department Biology II, Ludwig-Maximilians-University Munich, Großhadernerstr. 2, 82152, Planegg-Martinsried, Germany.
J Physiol. 2015 Apr 1;593(7):1685-700. doi: 10.1113/jphysiol.2014.282194. Epub 2015 Feb 19.
Hyperpolarization-activated non-specific cation-permeable channels (HCN) mediate I(H) currents, which are modulated by cGMP and cAMP and by nitric oxide (NO) signalling. Channel properties depend upon subunit composition (HCN1-4 and accessory subunits) as demonstrated in expression systems, but physiological relevance requires investigation in native neurons with intact intracellular signalling. Here we use the superior olivary complex (SOC), which exhibits a distinctive pattern of HCN1 and HCN2 expression, to investigate NO modulation of the respective I(H) currents, and compare properties in wild-type and HCN1 knockout mice. The medial nucleus of the trapezoid body (MNTB) expresses HCN2 subunits exclusively, and sends inhibitory projections to the medial and lateral superior olives (MSO, LSO) and the superior paraolivary nucleus (SPN). In contrast to the MNTB, these target nuclei possess an I(H) with fast kinetics, and they express HCN1 subunits. NO is generated in the SOC following synaptic activity and here we show that NO selectively suppresses HCN1, while enhancing IH mediated by HCN2 subunits. NO hyperpolarizes the half-activation of HCN1-mediated currents and slows the kinetics of native IH currents in the MSO, LSO and SPN. This modulation was independent of cGMP and absent in transgenic mice lacking HCN1. Independently, NO signalling depolarizes the half-activation of HCN2-mediated I(H) currents in a cGMP-dependent manner. Thus, NO selectively suppresses fast HCN1-mediated I(H) and facilitates a slow HCN2-mediated I(H) , so generating a spectrum of modulation, dependent on the local expression of HCN1 and/or HCN2.
超极化激活的非特异性阳离子通透通道(HCN)介导I(H)电流,该电流受环鸟苷酸(cGMP)、环磷酸腺苷(cAMP)以及一氧化氮(NO)信号通路的调节。正如在表达系统中所证实的,通道特性取决于亚基组成(HCN1 - 4和辅助亚基),但生理相关性需要在具有完整细胞内信号传导的天然神经元中进行研究。在这里,我们利用上橄榄复合体(SOC),其呈现出独特的HCN1和HCN2表达模式,来研究NO对各自I(H)电流的调节,并比较野生型和HCN1基因敲除小鼠的特性。梯形体内侧核(MNTB)仅表达HCN2亚基,并向内侧和外侧上橄榄核(MSO、LSO)以及上橄榄旁核(SPN)发送抑制性投射。与MNTB不同,这些靶核具有快速动力学的I(H),并且它们表达HCN1亚基。突触活动后,SOC中会产生NO,我们在此表明NO选择性地抑制HCN1,同时增强由HCN2亚基介导的I(H)电流。NO使HCN1介导电流的半激活超极化,并减缓MSO、LSO和SPN中天然I(H)电流的动力学。这种调节独立于cGMP,并且在缺乏HCN1的转基因小鼠中不存在。另外,NO信号通路以cGMP依赖的方式使HCN2介导的I(H)电流的半激活去极化。因此,NO选择性地抑制快速的HCN1介导的I(H),并促进缓慢的HCN2介导的I(H),从而产生一系列取决于HCN1和/或HCN2局部表达的调节作用。