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Slo家族通道的配体依赖性激活由可互换的胞质结构域所定义。

Ligand-dependent activation of Slo family channels is defined by interchangeable cytosolic domains.

作者信息

Xia Xiao-Ming, Zhang Xue, Lingle Christopher J

机构信息

Department of Anesthesiology, Washington University School of Medicine, St. Louis, Missouri 63110, USA.

出版信息

J Neurosci. 2004 Jun 16;24(24):5585-91. doi: 10.1523/JNEUROSCI.1296-04.2004.

Abstract

Large-conductance Ca2+- and voltage-regulated K+ channels (Slo1 BK-type) are controlled by two physiological stimuli, membrane voltage and cytosolic Ca2+. Regulation by voltage is similar to that in voltage-dependent K+ channels, arising from positively charged amino acids primarily within the S4 transmembrane helices. The basis for regulation by Ca2+ remains controversial. One viewpoint suggests that the extensive cytosolic C terminus contains the Ca2+ regulatory machinery, whereas another suggests that the pore-forming module contains the Ca2+-sensing elements. To address this issue, we take advantage of another Slo family member, the pH-regulated homolog Slo3. We reason that if the ligand-sensing apparatus is uniquely associated with a particular domain (either the pore or the cytosolic domain), exchange of those domains between Slo1 and Slo3 should result in exchange of ligand dependence in association with the key domain. The results show that the Slo3 cytosolic module confers pH-dependent regulation on the Slo1 pore module, whereas the Slo1 cytosolic module confers Ca2+-dependent regulation on the Slo3 pore module. Thus, ligand-specific regulation is defined by interchangeable cytosolic regulatory modules.

摘要

大电导钙激活钾通道(Slo1 BK型)受膜电位和胞质钙离子两种生理刺激的调控。电压调控机制与电压依赖性钾通道类似,主要源于S4跨膜螺旋内带正电荷的氨基酸。钙离子调控的机制仍存在争议。一种观点认为,广泛的胞质C末端包含钙离子调控机制,而另一种观点则认为,成孔模块包含钙离子感应元件。为解决这一问题,我们利用了Slo家族的另一个成员,即pH值调控的同系物Slo3。我们推断,如果配体感应装置与特定结构域(孔道结构域或胞质结构域)独特相关,那么Slo1和Slo3之间这些结构域的交换应导致与关键结构域相关的配体依赖性交换。结果表明,Slo3胞质模块赋予Slo1孔道模块pH依赖性调控,而Slo1胞质模块赋予Slo3孔道模块钙离子依赖性调控。因此,配体特异性调控由可互换的胞质调控模块决定。

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