首页> 美国卫生研究院文献>The Journal of Physiology >Kinetic evidence distinguishing volume-sensitive chloride current from other types in guinea-pig ventricular myocytes.
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Kinetic evidence distinguishing volume-sensitive chloride current from other types in guinea-pig ventricular myocytes.

机译:动力学证据将豚鼠心室肌​​细胞中体积敏感的氯离子电流与其他类型的氯离子电流区分开。

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摘要

1. Kinase-mediated chloride currents (ICl) in guinea-pig ventricular myocytes were activated by application of phorbol ester or forskolin, and compared with currents induced by hyposmotic swelling. Swelling-activated current was identified as ICl from changes in reversal potential, outward rectification and conductance when the Cl-gradient was modified. 2. Kinase-stimulated currents were relatively time and voltage independent, whereas hyposmotic swelling-stimulated (hyposmotic-stimulated) currents inactivated during 100 ms pulses to positive potentials. Forskolin stimulated time-independent ICl in myocytes with current unresponsive to hyposmotic superfusion, and superimposed a similar pedestal on time-dependent ICl in swollen myocytes. 3. Less negative holding potentials depressed hyposmotic-stimulated ICl tested at +80 mV; inhibition was half-maximal at -25 mV. Pulses from -80 to +80 mV inactivated up to 75% of ICl along a multi-exponential time course; repolarization elicited inwardly developing tail currents whose time courses suggest complex gating. 4. Hyperpolarizations, after strongly-inactivating depolarizations, triggered reactivating tail currents whose amplitude and configuration were dependent on voltage and Cl-gradients; tails were large and inwardly developing at potentials negative to the calculated Cl-equilibrium potential (ECl), small and outwardly developing at potentials positive to ECl, and time independent near ECl. 5. These results suggest that the volume-sensitive Cl- channels investigated here are distinct from other Cl- channels in guinea-pig ventricular myocytes. However, their voltage-dependent properties strongly resemble those of volume-sensitive Cl- channels in certain epithelial cells.
机译:1.通过应用佛波酯或毛喉素激活豚鼠心室肌​​细胞中激酶介导的氯离子电流(ICl),并将其与低渗性肿胀诱导的电流进行比较。根据Cl梯度的改变,通过反向电位,向外整流和电导的变化,将膨胀激活电流确定为ICl。 2.激酶刺激的电流相对于时间和电压是相对独立的,而低渗的溶胀刺激(低渗刺激)电流在100 ms脉冲期间失活为正电位。福斯高林刺激肌细胞中时间依赖性的ICl,而电流对低渗性充血无反应,并且在肿胀的肌细胞中的时间依赖性ICl上叠加了类似的基座。 3.在+80 mV下测得的负保持电位较低,抑制了低渗刺激的ICl。抑制在-25 mV时为最大值的一半。在多指数时间过程中,从-80到+80 mV的脉冲使多达75%的ICl失活;复极化引起向内发展的尾流,其时程表明复杂的门控。 4.在强烈失活的去极化作用之后,超极化触发了重新活化的尾电流,其幅度和构型取决于电压和Cl梯度;尾巴较大,向内发育,其电位对计算出的Cl平衡电位(EC1)为负;较小,向外向内发育,对ECl呈正电位,且时间独立于ECl。 5.这些结果表明,本文研究的对体积敏感的Cl-通道不同于豚鼠心室肌​​细胞中的其他Cl-通道。但是,它们的电压依赖性特性与某些上皮细胞中的体积敏感型Cl-通道非常相似。

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