We have investigated the role of the kinesin I isoform Kif5b in the trafficking of a cardiac voltage-gated potassium channel, Kv1.5. In Kv1.5-expressing HEK293 cells and H9c2 cardiomyoblasts, current densities were increased from control levels of 389 +/- 50.0 and 317 +/- 50.3 pA pF(1), respectively, to 614 +/- 74.3 and 580 +/- 90.9 pA pF(1) in cells overexpressing the Kif5b motor. Overexpression of the Kif5b motor increased Kv1.5 expression additively with several manipulations that reduce channel internalization, suggesting that it is involved in the delivery of the channel to the cell surface. In contrast, expression of a Kif5b dominant negative (Kif5bDN) construct increased Kv1.5 expression non-additively with these manipulations. Thus, the dominant negative acts by indirectly inhibiting endocytosis. The increase in Kv1.5 currents induced by wild-type Kif5b was dependent on Golgi function; a 6 h treatment with Brefeldin A reduced Kv1.5 currents to control levels in Kif5b-overexpressing cells but had little effect on the increase associated with Kif5bDN expression. Finally, expression of the Kif5bDN prior to induction of Kv1.5 in a tetracycline inducible system blocked surface expression of the channel in both HEK293 cells and H9c2 cardiomyoblasts. Thus, Kif5b is essential to anterograde trafficking of a cardiac voltage-gated potassium channel.
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机译:我们已经研究了驱动蛋白I亚型Kif5b在心脏电压门控钾通道Kv1.5的运输中的作用。在表达Kv1.5的HEK293细胞和H9c2心肌母细胞中,电流密度分别从控制水平389 +/- 50.0和317 +/- 50.3 pA pF(1)增加到614 +/- 74.3和580 +/-过表达Kif5b电机的细胞中90.9 pA pF(1)。 Kif5b马达的过度表达通过减少通道内部化的几种操作相加地增加了Kv1.5表达,这表明它参与了通道向细胞表面的传递。相反,通过这些操作,Kif5b显性负性(Kif5bDN)构建体的表达非可加性地增加了Kv1.5表达。因此,显性负性通过间接抑制内吞作用起作用。野生型Kif5b诱导的Kv1.5电流的增加取决于高尔基体功能。用布雷菲德菌素A处理6小时可降低Kv1.5电流,以控制过表达Kif5b的细胞中的水平,但对与Kif5bDN表达相关的增加影响很小。最后,在四环素可诱导系统中诱导Kv1.5之前,Kif5bDN的表达阻断了HEK293细胞和H9c2心肌母细胞中通道的表面表达。因此,Kif5b对心脏电压门控钾通道的顺行转运至关重要。
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