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前庭壶腹终末 hyperpolarization-activated current (I(h)):特征及其在塑造突触后事件中的作用。

Hyperpolarization-activated current (I(h)) in vestibular calyx terminals: characterization and role in shaping postsynaptic events.

机构信息

Neuroscience Program, University of Colorado School of Medicine, Aurora, CO 80045, USA.

出版信息

J Assoc Res Otolaryngol. 2012 Dec;13(6):745-58. doi: 10.1007/s10162-012-0342-3. Epub 2012 Jul 24.

Abstract

Calyx afferent terminals engulf the basolateral region of type I vestibular hair cells, and synaptic transmission across the vestibular type I hair cell/calyx is not well understood. Calyces express several ionic conductances, which may shape postsynaptic potentials. These include previously described tetrodotoxin-sensitive inward Na(+) currents, voltage-dependent outward K(+) currents and a K(Ca) current. Here, we characterize an inwardly rectifying conductance in gerbil semicircular canal calyx terminals (postnatal days 3-45), sensitive to voltage and to cyclic nucleotides. Using whole-cell patch clamp, we recorded from isolated calyx terminals still attached to their type I hair cells. A slowly activating, noninactivating current (I(h)) was seen with hyperpolarizing voltage steps negative to the resting potential. External Cs(+) (1-5 mM) and ZD7288 (100 μM) blocked the inward current by 97 and 83 %, respectively, confirming that I(h) was carried by hyperpolarization-activated, cyclic nucleotide gated channels. Mean half-activation voltage of I(h) was -123 mV, which shifted to -114 mV in the presence of cAMP. Activation of I(h) was well described with a third order exponential fit to the current (mean time constant of activation, τ, was 190 ms at -139 mV). Activation speeded up significantly (τ=136 and 127 ms, respectively) when intracellular cAMP and cGMP were present, suggesting that in vivo I(h) could be subject to efferent modulation via cyclic nucleotide-dependent mechanisms. In current clamp, hyperpolarizing current steps produced a time-dependent depolarizing sag followed by either a rebound afterdepolarization or an action potential. Spontaneous excitatory postsynaptic potentials (EPSPs) became larger and wider when I(h) was blocked with ZD7288. In a three-dimensional mathematical model of the calyx terminal based on Hodgkin-Huxley type ionic conductances, removal of I(h) similarly increased the EPSP, whereas cAMP slightly decreased simulated EPSP size and width.

摘要

花萼传入末端包绕 I 型前庭毛细胞的基底外侧区域,而前庭 I 型毛细胞/花萼之间的突触传递尚不清楚。花萼表达几种离子电导,这些电导可能会影响突触后电位。其中包括先前描述的河豚毒素敏感内向钠离子(Na+)电流、电压依赖性外向钾(K+)电流和 K(Ca)电流。在这里,我们描述了沙土鼠半规管花萼末端的内向整流电导(出生后 3-45 天),该电导对电压和环核苷酸敏感。通过全细胞膜片钳技术,我们从仍与其 I 型毛细胞相连的分离花萼末端进行记录。在超极化电压步骤负于静息电位时,观察到缓慢激活、非失活电流(I(h))。外部 Cs+(1-5 mM)和 ZD7288(100 μM)分别阻断内向电流 97%和 83%,证实 I(h)是由超极化激活、环核苷酸门控通道携带的。I(h)的平均半激活电压为-123 mV,在 cAMP 存在下,该电压移至-114 mV。I(h)的激活可以用电流的三阶指数拟合很好地描述(在-139 mV 时,激活的平均时间常数 τ 为 190 ms)。当细胞内 cAMP 和 cGMP 存在时,激活速度显著加快(τ 分别为 136 和 127 ms),这表明在体内,I(h)可能受到通过环核苷酸依赖机制的传出调制。在电流钳模式下,超极化电流阶跃产生时程依赖性去极化凹陷,随后是复发性后去极化或动作电位。当用 ZD7288 阻断 I(h)时,自发性兴奋性突触后电位(EPSP)变得更大和更宽。在基于 Hodgkin-Huxley 型离子电导的花萼末端三维数学模型中,去除 I(h)同样会增加 EPSP,而 cAMP 则略微减小模拟 EPSP 的大小和宽度。

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