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Inhibitory and excitatory neuromodulation by hydrogen peroxide: translating energetics to information

机译:过氧化氢的抑制性和兴奋性神经调节:将能量学转化为信息

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Historically, brain neurochemicals have been broadly classified as energetic or informational. However, increasing evidence implicates metabolic substrates and byproducts as signalling agents, which blurs the boundary between energy and information, and suggests the introduction of a new category for translational' substances that convey changes in energy state to information. One intriguing example is hydrogen peroxide (H2O2), which is a small, readily diffusible molecule. Produced during mitochondrial respiration, this reactive oxygen species, can mediate dynamic regulation of neuronal activity and transmitter release by activating inhibitory ATP-sensitive K+ (K-ATP) channels, as well as a class of excitatory non-selective cation channels, TRPM2. Studies using ex vivo guinea pig brain slices have revealed that activity-generated H2O2 can act via K-ATP channels to inhibit dopamine release in dorsal striatum and dopamine neuron activity in the substantia nigra pars compacta. In sharp contrast, endogenously generated H2O2 enhances the excitability of GABAergic projection neurons in the dorsal striatum and substantia nigra pars reticulata by activating TRPM2 channels. These studies suggest that the balance of excitation vs. inhibition produced in a given cell by metabolically generated H2O2 will be dictated by the relative abundance of H2O2-sensitive ion channel targets that receive this translational signal.
机译:从历史上看,脑神经化学物质已被广泛地分为精力充沛的或信息性的。但是,越来越多的证据表明代谢底物和副产物作为信号传递剂,这模糊了能量和信息之间的界限,并建议引入一种新类别的翻译物质来将能量状态的变化传达给信息。一个有趣的例子是过氧化氢(H2O2),它是一种小分子,易于扩散。线粒体呼吸过程中产生的这种活性氧可以通过激活抑制性ATP敏感的K +(K-ATP)通道以及一类兴奋性非选择性阳离子通道TRPM2来介导神经元活动和递质释放的动态调节。使用离体豚鼠脑片的研究表明,活性产生的H2O2可以通过K-ATP通道来抑制纹状体背侧纹状体中的多巴胺释放和黑质中的多巴胺神经元活性。与之形成鲜明对比的是,内源性生成的H2O2通过激活TRPM2通道增强了背侧纹状体和黑质网状结构中GABA能投射神经元的兴奋性。这些研究表明,代谢产生的H2O2在给定细胞中产生的激发与抑制之间的平衡将由接收该翻译信号的H2O2敏感离子通道靶的相对丰度决定。

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