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Properties and molecular basis of the mouse urinary bladder voltage-gated K+ current.

机译:小鼠膀胱电压门控K +电流的性质和分子基础。

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Potassium channels play an important role in controlling the excitability of urinary bladder smooth muscle (UBSM). Here we describe the biophysical, pharmacological and molecular properties of the mouse UBSM voltage-gated K+ current (IK(V)). The IK(V) activated, deactivated and inactivated slowly with time constants of 29.9 ms at +30 mV, 131 ms at -40 mV and 3.4 s at +20 mV. The midpoints of steady-state activation and inactivation curves were 1.1 mV and -61.4 mV, respectively. These properties suggest that IK(V) plays a role in regulating the resting membrane potential and contributes to the repolarization and after-hyperpolarization phases of action potentials. The IK(V) was blocked by tetraethylammonium ions with an IC50 of 5.2 mM and was unaffected by 1 mM 4-aminopyridine. RT-PCR for voltage-gated K+ channel (KV) subunits revealed the expression of Kv2.1, Kv5.1, Kv6.1, Kv6.2 and Kv6.3 in isolated UBSM myocytes. A comparison of the biophysical properties of UBSM IK(V) with those reported for Kv2.1 and Kv5.1 and/or Kv6 heteromultimeric channels demonstrated a marked similarity. We propose that heteromultimeric channel complexes composed of Kv2.1 and Kv5.1 and/or Kv6 subunits form the molecular basis of the mouse UBSM IK(V).
机译:钾通道在控制膀胱平滑肌(UBSM)的兴奋性中起重要作用。在这里,我们描述了鼠标UBSM电压门控K +电流(IK(V))的生物物理,药理和分子特性。 IK(V)缓慢地激活,去激活和去激活,其时间常数在+30 mV时为29.9 ms,在-40 mV时为131 ms,在+20 mV时为3.4 s。稳态激活和失活曲线的中点分别为1.1 mV和-61.4 mV。这些性质表明,IK(V)在调节静止膜电位中起作用,并有助于动作电位的复极化和超极化后阶段。 IK(V)被四乙铵离子封闭,IC50为5.2 mM,不受1 mM 4-氨基吡啶的影响。电压门控K +通道(KV)亚基的RT-PCR显示了分离的UBSM心肌细胞中Kv2.1,Kv5.1,Kv6.1,Kv6.2和Kv6.3的表达。 UBSM IK(V)的生物物理特性与Kv2.1和Kv5.1和/或Kv6异源多聚体通道报道的生物物理特性的比较显示出明显的相似性。我们建议由Kv2.1和Kv5.1和/或Kv6亚基组成的异源多聚体通道复合物形成小鼠UBSM IK(V)的分子基础。

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