Although the biophysical fingerprints (ion selectivity, voltage-dependence, kinetics, etc) of Ca(2+)-activated Cl(-) currents are well established, their molecular identity is still controversial. Several molecular candidates have been suggested; however, none of them has been fully accepted. We have recently characterized a cGMP-dependent Ca(2+)-activated Cl(-) current with unique characteristics in smooth muscle cells. This novel current has been shown to coexist with a "classic" (cGMP-independent) Ca(2+)-activated Cl(-) current and to have characteristics distinct from those previously known for Ca(2+)-activated Cl(-) currents. Here, we suggest that a bestrophin, a product of the Best gene family, is responsible for the cGMP-dependent Ca(2+)-activated Cl(-) current based on similarities between the membrane currents produced by heterologous expressions of bestrophins and the cGMP-dependent Ca(2+)-activated Cl(-) current. This is supported by similarities in the distribution pattern of the cGMP-dependent Ca(2+)-activated Cl(-) current and bestrophin-3 (the product of Best-3 gene) expression in different smooth muscle. Furthermore, downregulation of Best-3 gene expression with small interfering RNA both in cultured cells and in vascular smooth muscle cells in vivo was associated with a significant reduction of the cGMP-dependent Ca(2+)-activated Cl(-) current, whereas the magnitude of the classic Ca(2+)-activated Cl(-) current was not affected. The majority of previous suggestions that bestrophins are a new Cl(-) channel family were based on heterologous expression in cell culture studies. Our present results demonstrate that at least 1 family member, bestrophin-3, is essential for a well-defined endogenous Ca(2+)-activated Cl(-) current in smooth muscles in the intact vascular wall.

译文

:尽管Ca(2)激活的Cl(-)电流的生物物理指纹(离子选择性,电压依赖性,动力学等)已被很好地建立,但它们的分子身份仍然存在争议。已经提出了几种分子候选物。但是,它们都没有被完全接受。我们最近表征了cGMP依赖性Ca(2)激活Cl(-)当前具有在平滑肌细胞中的独特特征。该新型电流已显示与“经典”(独立于cGMP的)Ca(2)激活的Cl(-)电流共存,并且具有不同于先前已知的Ca(2)激活的Cl(-)电流的特性。 。在这里,我们建议Bestrophin,最好的基因家族的产物,负责由cGMP依赖Ca(2)激活的Cl(-)电流,这取决于Bestrophins与cGMP的异源表达所产生的膜电流之间的相似性。依赖的Ca(2)激活的Cl(-)电流。这由cGMP依赖性Ca(2)激活的Cl(-)电流和Bestrophin-3(Best-3基因的产物)表达在不同平滑肌中的分布模式的相似性所支持。此外,在体内培养的细胞和血管平滑肌细胞中的小干扰RNA的Best-3基因表达的下调与cGMP依赖性Ca(2)激活的Cl(-)电流的显着降低有关,而的经典Ca(2)激活Cl(-)电流的大小不受影响。以前的大多数建议,即最佳动物生长素是一个新的Cl(-)通道家族,是基于细胞培养研究中的异源表达。我们目前的结果表明,至少1个家庭成员,Bestrophin-3,对于完整血管壁平滑肌中明确定义的内源性Ca(2)激活Cl(-)电流是必不可少的。

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