首页> 外文期刊>Molecular and Cellular Biochemistry >Involvement of rhodopsin and ATP in the activation of membranous guanylate cyclase in retinal photoreceptor outer segments (ROS-GC) by GC-activating proteins (GCAPs): a new model for ROS-GC activation and its link to retinal diseases
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Involvement of rhodopsin and ATP in the activation of membranous guanylate cyclase in retinal photoreceptor outer segments (ROS-GC) by GC-activating proteins (GCAPs): a new model for ROS-GC activation and its link to retinal diseases

机译:视紫红质和ATP参与GC激活蛋白(GCAPs)激活视网膜感光细胞外段(ROS-GC)的膜型鸟苷酸环化酶:ROS-GC激活的新模型及其与视网膜疾病的联系

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摘要

Membranous guanylate cyclase in retinal photoreceptor outer segments (ROS-GC), a key enzyme for the recovery of photoreceptors to the dark state, has a topology identical to and cytoplasmic domains homologous to those of peptide-regulated GCs. However, under the prevailing concept, its activation mechanism is significantly different from those of peptide-regulated GCs: GC-activating proteins (GCAPs) function as the sole activator of ROS-GC in a Ca2+-sensitive manner, and neither reception of an outside signal by the extracellular domain (ECD) nor ATP binding to the kinase homology domain (KHD) is required for its activation. We have recently shown that ATP pre-binding to the KHD in ROS-GC drastically enhances its GCAP-stimulated activity, and that rhodopsin illumination, as the outside signal, is required for the ATP pre-binding. These results indicate that illuminated rhodopsin is involved in ROS-GC activation in two ways: to initiate ATP binding to ROS-GC for preparation of its activation and to reduce [Ca2+] through activation of cGMP phosphodiesterase. These two signal pathways are activated in a parallel and proportional manner and finally converge for strong activation of ROS-GC by Ca2+-free GCAPs. These results also suggest that the ECD receives the signal for ATP binding from illuminated rhodopsin. The ECD is projected into the intradiscal space, i.e., an intradiscal domain(s) of rhodopsin is also involved in the signal transfer. Many retinal disease-linked mutations are found in these intradiscal domains; however, their consequences are often unclear. This model will also provide novel insights into causal relationship between these mutations and certain retinal diseases. Keywords Retinal photoreceptor membrane guanylate cyclase - Rhodopsin - ATP-binding protein - GCAPs - Retinitis pigmentosa - Leber’s congenital amaurosis
机译:视网膜光感受器外部节段(ROS-GC)中的膜状鸟苷酸环化酶是一种将光感受器恢复到黑暗状态的关键酶,其拓扑结构与肽调节的GC相同且胞质结构域同源。然而,在普遍的概念下,其激活机制与肽调节的GC的激活机制明显不同:GC激活蛋白(GCAP)在Ca 2 + -中充当ROS-GC的唯一激活剂。激活方式既不需要细胞外结构域(ECD)接收外部信号,也不需要ATP结合激酶同源结构域(KHD)。我们最近显示,在ROS-GC中,ATP与KHD的预结合可大大增强其GCAP刺激的活性,并且视紫红质的照明作为外部信号,是ATP预结合所必需的。这些结果表明光照的视紫红质以两种方式参与ROS-GC的活化:启动ATP与ROS-GC的结合以制备其活化作用以及通过激活cGMP磷酸二酯酶来减少[Ca 2 + ] 。这两个信号通路以平行和成比例的方式被激活,并最终收敛为无Ca 2 + 的GCAP对ROS-GC的强激活。这些结果还表明,ECD从发光的视紫红质中接收到ATP结合信号。 ECD投射到椎间盘间隙中,即视紫红质的椎间盘内域也参与信号传递。在这些椎间盘内结构域中发现了许多与视网膜疾病相关的突变。但是,它们的后果通常不清楚。该模型还将为这些突变与某些视网膜疾病之间的因果关系提供新颖的见解。关键词视网膜感光膜鸟苷酸环化酶-视紫红质-ATP结合蛋白-GCAPs-色素性视网膜炎-莱伯先天性黑病

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