首页> 美国卫生研究院文献>The Journal of Biological Chemistry >Distinct domains of the β1-subunit cytosolic N terminus control surface expression and functional properties of large-conductance calcium-activated potassium (BK) channels
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Distinct domains of the β1-subunit cytosolic N terminus control surface expression and functional properties of large-conductance calcium-activated potassium (BK) channels

机译:β1亚基胞质N末端的不同域控制大电导钙激活钾(BK)通道的表面表达和功能特性

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摘要

The properties and function of large-conductance calcium- and voltage-activated potassium (BK) channels are modified by the tissue-specific expression of regulatory β1-subunits. Although the short cytosolic N-terminal domain of the β1-subunit is important for controlling both BK channel trafficking and function, whether the same, or different, regions of the N terminus control these distinct processes remains unknown. Here we demonstrate that the first six N-terminal residues including Lys-3, Lys-4, and Leu-5 are critical for controlling functional regulation, but not trafficking, of BK channels. This membrane-distal region has features of an amphipathic helix that is predicted to control the orientation of the first transmembrane-spanning domain (TM1) of the β1-subunit. In contrast, a membrane-proximal leucine residue (Leu-17) controls trafficking without affecting functional coupling, an effect that is in part dependent on controlling efficient endoplasmic reticulum exit of the pore-forming α-subunit. Thus cell surface trafficking and functional coupling with BK channels are controlled by distinct domains of the β1-subunit N terminus.
机译:大电导钙和电压激活的钾(BK)通道的特性和功能通过调节性β1亚基的组织特异性表达而改变。尽管β1亚基的短胞质N末端结构域对于控制BK通道运输和功能都很重要,但无论N端区域相同还是不同,这些不同的过程仍然未知。在这里,我们证明了包括Lys-3,Lys-4和Leu-5在内的前六个N端残基对于控制BK通道的功能调节(而非贩运)至关重要。该膜远端区域具有两亲性螺旋的特征,预计可控制β1亚基的第一个跨膜结构域(TM1)的方向。相反,膜近端亮氨酸残基(Leu-17)控制运输而不影响功能偶联,这种作用部分取决于控制成孔α亚基的有效内质网出口。因此,细胞表面运输和与BK通道的功能性耦合受β1-亚基N末端不同域的控制。

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