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膜鸟苷酸环化酶复合物塑造视网膜视杆细胞和视锥细胞的光反应。

Membrane guanylyl cyclase complexes shape the photoresponses of retinal rods and cones.

作者信息

Wen Xiao-Hong, Dizhoor Alexander M, Makino Clint L

机构信息

Department of Ophthalmology, Massachusetts Eye and Ear Infirmary and Harvard Medical School Boston, MA, USA.

Department of Basic Sciences Research and Pennsylvania College of Optometry, Salus University Elkins Park, PA, USA.

出版信息

Front Mol Neurosci. 2014 Jun 2;7:45. doi: 10.3389/fnmol.2014.00045. eCollection 2014.

Abstract

In vertebrate rods and cones, photon capture by rhodopsin leads to the destruction of cyclic GMP (cGMP) and the subsequent closure of cyclic nucleotide gated ion channels in the outer segment plasma membrane. Replenishment of cGMP and reopening of the channels limit the growth of the photon response and are requisite for its recovery. In different vertebrate retinas, there may be as many as four types of membrane guanylyl cyclases (GCs) for cGMP synthesis. Ten neuronal Ca(2+) sensor proteins could potentially modulate their activities. The mouse is proving to be an effective model for characterizing the roles of individual components because its relative simplicity can be reduced further by genetic engineering. There are two types of GC activating proteins (GCAPs) and two types of GCs in mouse rods, whereas cones express one type of GCAP and one type of GC. Mutant mouse rods and cones bereft of both GCAPs have large, long lasting photon responses. Thus, GCAPs normally mediate negative feedback tied to the light-induced decline in intracellular Ca(2+) that accelerates GC activity to curtail the growth and duration of the photon response. Rods from other mutant mice that express a single GCAP type reveal how the two GCAPs normally work together as a team. Because of its lower Ca(2+) affinity, GCAP1 is the first responder that senses the initial decrease in Ca(2+) following photon absorption and acts to limit response amplitude. GCAP2, with a higher Ca(2+) affinity, is recruited later during the course of the photon response as Ca(2+) levels continue to decline further. The main role of GCAP2 is to provide for a timely response recovery and it is particularly important after exposure to very bright light. The multiplicity of GC isozymes and GCAP homologs in the retinas of other vertebrates confers greater flexibility in shaping the photon responses in order to tune visual sensitivity, dynamic range and frequency response.

摘要

在脊椎动物的视杆细胞和视锥细胞中,视紫红质捕获光子会导致环磷酸鸟苷(cGMP)的破坏,随后外段质膜中的环核苷酸门控离子通道关闭。cGMP的补充和通道的重新开放限制了光子反应的增长,是其恢复所必需的。在不同的脊椎动物视网膜中,可能有多达四种类型的膜鸟苷酸环化酶(GCs)用于cGMP合成。十种神经元钙(Ca2+)传感器蛋白可能会调节它们的活性。事实证明,小鼠是表征单个成分作用的有效模型,因为通过基因工程可以进一步降低其相对简单性。小鼠视杆细胞中有两种类型的GC激活蛋白(GCAPs)和两种类型的GCs,而视锥细胞则表达一种类型的GCAP和一种类型的GC。缺乏两种GCAPs的突变小鼠视杆细胞和视锥细胞具有大的、持久的光子反应。因此,GCAPs通常介导与光诱导的细胞内Ca2+下降相关的负反馈,加速GC活性以缩短光子反应的增长和持续时间。来自表达单一GCAP类型的其他突变小鼠的视杆细胞揭示了两种GCAPs通常如何作为一个团队协同工作。由于其较低的Ca2+亲和力,GCAP1是第一个响应者,它感知光子吸收后Ca2+的初始下降,并作用于限制反应幅度。具有较高Ca2+亲和力的GCAP2在光子反应过程中稍后随着Ca2+水平继续进一步下降而被招募。GCAP2的主要作用是提供及时的反应恢复,在暴露于非常明亮的光后尤为重要。其他脊椎动物视网膜中GC同工酶和GCAP同源物的多样性赋予了在塑造光子反应方面更大的灵活性,以便调节视觉敏感性、动态范围和频率响应。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/87ae/4040495/8ca7d4d55364/fnmol-07-00045-g001.jpg

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