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首页> 外文期刊>American Journal of Physiology >Basally activated nonselective cation currents regulate the resting membrane potential in human and monkey colonic smooth muscle.
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Basally activated nonselective cation currents regulate the resting membrane potential in human and monkey colonic smooth muscle.

机译:基本活化的非选择性阳离子电流调节人和猴结肠平滑肌中的静止膜电位。

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摘要

Resting membrane potential (RMP) plays an important role in determining the basal excitability of gastrointestinal smooth muscle. The RMP in colonic muscles is significantly less negative than the equilibrium potential of K(+), suggesting that it is regulated not only by K(+) conductances but by inward conductances such as Na(+) and/or Ca(2+). We investigated the contribution of nonselective cation channels (NSCC) to the RMP in human and monkey colonic smooth muscle cells (SMC) using voltage- and current-clamp techniques. Qualitative reverse transcriptase-polymerase chain reaction was performed to examine potential molecular candidates for these channels among the transient receptor potential (TRP) channel superfamily. Spontaneous transient inward currents and holding currents were recorded in human and monkey SMC. Replacement of extracellular Na(+) with equimolar tetraethylammonium or Ca(2+) with Mn(2+) inhibited basally activated nonselective cation currents. Trivalent cations inhibited these channels. Under current clamp, replacement of extracellular Na(+) with N-methyl-D-glucamine or addition of trivalent cations caused hyperpolarization. Three unitary conductances of NSCC were observed in human and monkey colonic SMC. Molecular candidates for basally active NSCC were TRPC1, C3, C4, C7, M2, M4, M6, M7, V1, and V2 in human and monkey SMC. Comparison of the biophysical properties of these TRP channels with basally active NSCC (bI(NSCC)) suggests that TRPM4 and specific TRPC heteromultimer combinations may underlie the three single-channel conductances of bI(NSCC). In conclusion, these findings suggest that basally activated NSCC contribute to the RMP in human and monkey colonic SMC and therefore may play an important role in determining basal excitability of colonic smooth muscle.
机译:休息膜电位(RMP)在确定胃肠道平滑肌的基础兴奋性方面发挥着重要作用。结肠肌的RMP比K(+)的平衡电位显着低得多,表明它不仅由K(+)电导而调节,而是通过内向导电(例如Na(+)和/或Ca(2+) 。我们使用电压和电流钳技术调查了非选择性阳离子通道(NSCC)对人和猴结肠平滑肌细胞(SMC)的RMP的贡献。进行定性逆转录酶聚合酶链反应,以检查瞬态受体电位(TRP)通道中的这些通道的潜在分子候选。在人和猴子SMC中记录了自发的瞬态向内电流和持有电流。用Mn(2+)的等摩尔四乙基铵或Ca(2+)的细胞外Na(+)抑制基本活化的非选择性阳离子电流。三价阳离子抑制了这些渠道。在电流夹层下,用N-甲基-D-葡聚糖的替代细胞外Na(+)或添加三价阳离子引起超极化。在人和猴结肠SMC中观察到NSCC的三种整体电导。用于基础活性NSCC的分子候选者是人和猴子SMC中的TRPC1,C3,C4,C7,M2,M4,M6,M7,V1和V2。这些TRP通道与基本有源NSCC(BI(NSCC))的生物物理特性的比较表明TRPM4和特定的TRPC异常组合可以利于BI(NSCC)的三个单通道电导。总之,这些研究结果表明,基本活化的NSCC在人和猴结肠SMC中有助于RMP,因此可能在确定结肠平滑肌的基础兴奋性方面发挥重要作用。

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