Ueda Atsushi, Wu Chun-Fang
Department of Biological Sciences, University of Iowa, Iowa City, Iowa 52242, USA.
J Neurogenet. 2008;22(2):1-13. doi: 10.1080/01677060701807954.
The Drosophila Hyperkinetic (Hk) gene encodes a beta subunit of Shaker (Sh) K+ channels and shows high sequence homology to aldoketoreductase. Hk mutations are known to modify the voltage dependence and kinetics of Sh currents, which are also influenced by the oxidative state of the N-terminus region of the Sh channel, as demonstrated in heterologous expression experiments in frog oocytes. However, an in vivo role of Hk in cellular reduction/oxidation (redox) has not been demonstrated. By using a fluorescent indicator of reactive oxygen species (ROS), dihydrorhodamine-123 (DHR), we show that the presynaptic nerve terminal of larval motor axons is metabolically active, with more rapid accumulation of ROS in comparison with muscle cells. In Hk terminals, DHR fluorescence was greatly enhanced, indicating increased ROS levels. This observation implicates a role of the Hk beta subunit in redox regulation in presynaptic terminals. This phenomenon was paralleled by the expected effects of the mutations affecting glutathione S-transferase S1 as well as applying H2O2 to wild-type synaptic terminals. Thus, our results also establish DHR as a useful tool for detecting ROS levels in the Drosophila neuromuscular junction.
果蝇的“多动”(Hk)基因编码Shaker(Sh)钾离子通道的一个β亚基,并且与醛酮还原酶具有高度的序列同源性。已知Hk突变会改变Sh电流的电压依赖性和动力学,正如在蛙卵母细胞的异源表达实验中所证明的,Sh电流也受Sh通道N端区域氧化状态的影响。然而,Hk在细胞还原/氧化(氧化还原)中的体内作用尚未得到证实。通过使用活性氧(ROS)荧光指示剂二氢罗丹明-123(DHR),我们发现幼虫运动轴突的突触前神经末梢具有代谢活性,与肌肉细胞相比,ROS积累更快。在Hk末梢中,DHR荧光大大增强,表明ROS水平升高。这一观察结果表明Hkβ亚基在突触前末梢的氧化还原调节中发挥作用。影响谷胱甘肽S-转移酶S1的突变以及将H2O2应用于野生型突触末梢所产生的预期效果与此现象相似。因此,我们的结果也确立了DHR作为检测果蝇神经肌肉接头处ROS水平的有用工具。