Institute for Physiology and Pathophysiology, Vegetative Physiology, Philipps University Marburg, Marburg, 35037, Germany.
Biochemistry (Mosc). 2011 Aug;76(8):890-9. doi: 10.1134/S0006297911080049.
The regulation of neuronal excitability is complex, as ion channels and neurotransmitter receptors are underlying a large variety of modulating effects. Alterations in the expression patterns of receptors or channel subunits as well as differential splicing contribute to the regulation of neuronal excitability. RNA editing is another and more recently explored mechanism to increase protein diversity, as the genomic recoding leads to new gene products with novel functional and pharmacological properties. In humans A-to-I RNA editing targets several neuronal receptors and channels, including GluR2/5/6 subunits, the Kv1.1 channel, and the 5-HT(2C) receptor. Our review summarizes that RNA editing of these proteins does not only change protein function, but also the pharmacology and presumably the drug therapy in human diseases.
神经元兴奋性的调节非常复杂,因为离子通道和神经递质受体是多种调节效应的基础。受体或通道亚基表达模式的改变以及差异剪接有助于调节神经元兴奋性。RNA 编辑是另一种更近期探索的增加蛋白质多样性的机制,因为基因组重编码导致具有新功能和药理学特性的新基因产物。在人类中,A-to-I RNA 编辑的靶标包括几个神经元受体和通道,包括 GluR2/5/6 亚基、Kv1.1 通道和 5-HT(2C)受体。我们的综述总结了这些蛋白质的 RNA 编辑不仅改变了蛋白质功能,还改变了人类疾病中的药理学和药物治疗。
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