首页> 外文期刊>American Journal of Physiology >Characteristics of single large-conductance Ca2+-activated K+ channels and their regulation of action potentials and excitability in parasympathetic cardiac motoneurons in the nucleus ambiguus
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Characteristics of single large-conductance Ca2+-activated K+ channels and their regulation of action potentials and excitability in parasympathetic cardiac motoneurons in the nucleus ambiguus

机译:单个大电导Ca2 +激活的K +通道的特征及其对副核交感神经运动神经元中动作电位和兴奋性的调节

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摘要

Large-conductance Ca2+-activated K+ channels (BK) regulate action potential (AP) properties and excitability in many central neurons. However, the properties and functional roles of BK channels in parasympathetic cardiac motoneurons (PCMNs) in the nucleus ambiguus (NA) have not yet been well characterized. In this study, the tracer Xrhodamine- 5 (and 6)-isothiocyanate (XRITC) was injected into the pericardial sac to retrogradely label PCMNs in FVB mice at postnatal 7-9 days. Two days later, XRITC-labeled PCMNs in brain stem slices were identified. Using excised patch single-channel recordings, we identified voltage-gated and Ca2+-dependent BK channels in PCMNs. The majority of BK channels exhibited persistent channel opening during voltage holding. These BK channels had a conductance of 237 pS and a 50% opening probability at +27.9 mV, the channel open time constant was 3.37 ms at +20 mV, and dwell time increased exponentially as the membrane potential depolarized. At the +20-mV holding potential, the [Ca2+]50 was 15.2 μM with a P0.5 of 0.4. Occasionally, some BK channels showed a transient channel opening and fast inactivation. Using whole cell voltage clamp, we found that BK channel mediated outward currents and afterhyperpolarization currents (IAHP). Using whole cell current clamp, we found that application of BK channel blocker iberiotoxin (IBTX) increased spike half-width and suppressed fast afterhyperpolarization (fAHP) amplitude following single APs. In addition, IBTX application increased spike half-width and reduced the spike frequency-dependent AP broadening in trains and spike frequency adaption (SFA). Furthermore, BK channel blockade decreased spike frequency. Collectively, these results demonstrate that PCMNs have BK channels that significantly regulate AP repolarization, fAHP, SFA, and spike frequency. We conclude that activation of BK channels underlies one of the mechanisms for facilitation of PCMN excitability.
机译:大电导的Ca2 +激活的K +通道(BK)调节许多中枢神经元的动作电位(AP)特性和兴奋性。但是,BK通道的性质和功能作用在副核(NA)副交感神经运动神经元(PCMNs)中。在这项研究中,示踪剂Xrhodamine-5(和6)-异硫氰酸酯(XRITC)被注射到心包囊中,以在出生后7-9天逆行标记FVB小鼠中的PCMNs。两天后,在脑干切片中鉴定出XRITC标记的PCMN。使用切除的贴片单通道录音,我们在PCMNs中确定了电压门控和依赖Ca2 +的BK通道。大多数BK通道在电压保持期间均显示出持久的通道打开状态。这些BK通道的电导率为237 pS,在+27.9 mV时的打开概率为50%,在+20 mV时的通道打开时间常数为3.37 ms,并且随着膜电位去极化,驻留时间呈指数增长。在+20 mV保持电势下,[Ca2 +] 50为15.2μM,P0.5为0.4。有时,某些BK通道显示出瞬时通道打开和快速失活。使用全细胞电压钳,我们发现BK通道介导向外电流和超极化后电流(IAHP)。使用全细胞电流钳,我们发现BK通道阻滞剂埃博毒素(IBTX)的应用增加了尖峰半峰宽度,并抑制了单个AP后的快速超极化(fAHP)幅度。此外,IBTX应用增加了尖峰半宽度,并减少了与尖峰频率相关的AP在列车中的拓宽和尖峰频率适应(SFA)。此外,BK通道封锁降低了尖峰频率。总的来说,这些结果表明PCMN具有BK通道,可以显着调节AP复极化,fAHP,SFA和尖峰频率。我们得出结论,BK通道的激活是促进PCMN兴奋性的机制之一。

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