GtoPdb v.2023.1中的环核苷酸调节通道(CNG)

Elvir Becirovic, Martin Biel, Stefanie Fenske, Verena Hammelmann, Franz Hofmann, U. Benjamin Kaupp
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摘要

环状核苷酸门控(CNG)通道在脊椎动物视觉和嗅觉系统的初级感觉细胞中负责信号传导。CNG通道是电压无关的阳离子通道,形成四聚体。每个亚基有6TM,成孔结构域位于TM5和TM6之间。CNG通道最早在杆状光感受器中被发现[83,120],光信号通过视紫红质和转导蛋白刺激磷酸二酯酶,降低细胞内环GMP水平。这将导致天然气通道的关闭和“暗电流”的减少。在嗅觉神经元的纤毛[181]和松果体[71]中也发现了类似的通道。环核苷酸与亚基蛋白C端的结构域结合:其他直接结合环核苷酸的通道包括高极化激活、环核苷酸门控通道(HCN)、醚-a-go-go通道和某些植物钾通道。HCN通道是阳离子通道,在负至~-50 mV的电压下被超极化激活。环核苷酸环AMP和环GMP直接结合到HCN通道的环核苷酸结合区域,使其激活曲线向更正的电压移动,从而增强通道活性。HCN通道是许多可兴奋细胞(包括心肌细胞和神经元)中的起搏器电流的基础[65,192]。在原生细胞中,这些电流有各种各样的名称,如Ih、Iq和If。已知的4个HCN通道具有6个跨膜结构域并形成四聚体。这些通道可以相互形成异构体,如HCN1和HCN4[2]。通过对CNG和HCN通道的高分辨率结构研究,可以深入了解这些通道的门控过程[139,146,140]。CNG和HCN通道的标准化命名已经由NC-IUPHAR电压门控离子通道小组委员会提出[108]。
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Cyclic nucleotide-regulated channels (CNG) in GtoPdb v.2023.1
Cyclic nucleotide-gated (CNG) channels are responsible for signalling in the primary sensory cells of the vertebrate visual and olfactory systems. CNG channels are voltage-independent cation channels formed as tetramers. Each subunit has 6TM, with the pore-forming domain between TM5 and TM6. CNG channels were first found in rod photoreceptors [83, 120], where light signals through rhodopsin and transducin to stimulate phosphodiesterase and reduce intracellular cyclic GMP level. This results in a closure of CNG channels and a reduced ‘dark current’. Similar channels were found in the cilia of olfactory neurons [181] and the pineal gland [71]. The cyclic nucleotides bind to a domain in the C terminus of the subunit protein: other channels directly binding cyclic nucleotides include hyperolarisation-activated, cyclic nucleotide-gated channels (HCN), ether-a-go-go and certain plant potassium channels.The HCN channels are cation channels that are activated by hyperpolarisation at voltages negative to ~-50 mV. The cyclic nucleotides cyclic AMP and cyclic GMP directly bind to the cyclic nucleotide-binding domain of HCN channels and shift their activation curves to more positive voltages, thereby enhancing channel activity. HCN channels underlie pacemaker currents found in many excitable cells including cardiac cells and neurons [65, 192]. In native cells, these currents have a variety of names, such as Ih, Iq and If. The four known HCN channels have six transmembrane domains and form tetramers. It is believed that the channels can form heteromers with each other, as has been shown for HCN1 and HCN4 [2]. High resolution structural studies of CNG and HCN channels has provided insight into the the gating processes of these channels [139, 146, 140]. A standardised nomenclature for CNG and HCN channels has been proposed by the NC-IUPHAR Subcommittee on voltage-gated ion channels [108].
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