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Spontaneous and neurally activated depolarizations in smooth muscle cells of the guinea-pig urethra

机译:豚鼠尿道平滑肌细胞的自发和神经激活去极化

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class="enumerated" style="list-style-type:decimal">Membrane potential recordings were made from longitudinal smooth muscle cells of the guinea-pig urethra using conventional microelectrode techniques.Smooth muscle cells of the urethra developed spontaneous transient depolarizations (STDs) and slow waves. Single unit STDs had amplitudes of approximately 5 mV and slow waves seemed to occur as amplitude multiples of single unit STDs.STDs and slow waves were abolished by niflumic acid or low chloride solution and also by cyclopiazonic acid (CPA), BAPTA or high concentrations of caffeine. Lower concentrations of caffeine abolished slow waves but not STDs. Nifedipine inhibited slow waves but not STDs.When stochastic properties of STDs were examined, it was found that the intervals between occurrences were not well modelled by Poisson statistics, instead the STDs appeared to be clustered.Transmural stimulation evoked excitatory junctional potentials (EJPs) and triggered slow waves which were abolished by either α,β-methylene-ATP or tetrodotoxin. Evoked slow waves were also abolished by caffeine, co-application of caffeine and ryanodine or by CPA which left EJPs unaffected.In conclusion, smooth muscle cells of urethra exhibit STDs which are clustered rather than random events, and are the result of spontaneous Ca2+ release from intracellular stores and subsequent activation of Ca2+-activated chloride channels. STDs sum to activate L-type Ca2+ channels which contribute to the sustained phase of slow waves. Stimulation of purinoceptors by neurally released ATP initiates EJPs and also causes the release of Ca2+ from intracellular stores to evoke slow waves.
机译:class =“ enumerated” style =“ list-style-type:decimal”> <!-list-behavior =枚举前缀-word = mark-type = decimal max-label-size = 0-> 使用传统的微电极技术,通过豚鼠尿道的纵向平滑肌细胞进行膜电位记录。 尿道的平滑肌细胞会产生自发的瞬时去极化(STD)和慢波。单单位STD的振幅大约为5 mV,并且似乎是单单位STD的振幅倍数出现慢波。 STD和慢波被烟酸或低氯化物溶液以及环吡嗪酸(CPA)废除了),BAPTA或高浓度的咖啡因。较低浓度的咖啡因可消除慢波,但不能消除性病。硝苯地平抑制慢波,但不抑制性传播疾病。 检查性传播疾病的随机特性时,发现泊松事件之间的间隔不能很好地通过泊松统计来建模,相反,性传播疾病似乎是聚类的。 总而言之,尿道平滑肌细胞表现出STD呈簇状而非随机事件,并且是细胞内存储自发释放Ca 2 + 以及随后激活Ca 2 + 激活的氯离子通道的结果。 STD共同激活L型Ca 2 + 通道,这些通道有助于慢波的持续相位。神经释放的ATP刺激嘌呤受体会引发EJP,并引起Ca 2 + 从细胞内存储中释放,从而引起慢波。

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