首页> 美国卫生研究院文献>Frontiers in Cellular Neuroscience >The Roles of Rods Cones and Melanopsin in Photoresponses of M4 Intrinsically Photosensitive Retinal Ganglion Cells (ipRGCs) and Optokinetic Visual Behavior
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The Roles of Rods Cones and Melanopsin in Photoresponses of M4 Intrinsically Photosensitive Retinal Ganglion Cells (ipRGCs) and Optokinetic Visual Behavior

机译:杆锥和黑皮素在M4本征光敏性视网膜神经节细胞(ipRGCs)和光动力学的视觉行为的光响应中的作用。

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摘要

Intrinsically photosensitive retinal ganglion cells (ipRGCs) mediate not only image-forming vision like other ganglion cells, but also non-image-forming physiological responses to light such as pupil constriction and circadian photoentrainment. All ipRGCs respond to light through their endogenous photopigment melanopsin as well as rod/cone-driven synaptic inputs. A major knowledge gap is how melanopsin, rods, and cones differentially drive ipRGC photoresponses and image-forming vision. We whole-cell-recorded from M4-type ipRGCs lacking melanopsin, rod input, or cone input to dissect the roles of each component in ipRGCs' responses to steady and temporally modulated (≥0.3 Hz) lights. We also used a behavioral assay to determine how the elimination of melanopsin, rod, or cone function impacts the optokinetic visual behavior of mice. Results showed that the initial, transient peak in an M4 cell's responses to 10-s light steps arises from rod and cone inputs. Both the sustainability and poststimulus persistence of these light-step responses depend only on rod and/or cone inputs, which is unexpected because these ipRGC photoresponse properties have often been attributed primarily to melanopsin. For temporally varying stimuli, the enhancement of response sustainedness involves melanopsin, whereas stimulus tracking is mediated by rod and cone inputs. Finally, the behavioral assay showed that while all three photoreceptive systems are nearly equally important for contrast sensitivity, only cones and rods contribute to spatial acuity.
机译:本质上,光敏性视网膜神经节细胞(ipRGC)不仅像其他神经节细胞一样介导图像形成视觉,还介导对光的非图像形成生理反应,例如瞳孔收缩和昼夜节律性光合。所有ipRGC均通过其内源性光色素黑素和杆/锥驱动的突触输入对光作出反应。一个主要的知识空白是黑视蛋白,视杆和视锥细胞如何差异性驱动ipRGC光响应和图像形成视觉。我们从缺乏黑素,杆输入或锥输入的M4型ipRGC进行全细胞记录,以剖析ipRGC对稳定和临时调制(≥0.3 Hz)光的响应中每个组件的作用。我们还使用行为分析来确定黑色素,棒或视锥细胞功能的消除如何影响小鼠的视动视觉行为。结果显示,M4电池对10 s光阶跃的响应中的初始瞬态峰值来自杆和锥输入。这些光阶响应的可持续性和刺激后持久性都仅取决于杆和/或锥输入,这是出乎意料的,因为这些ipRGC光响应特性通常主要归因于黑色素。对于随时间变化的刺激,反应持续性的增强涉及黑色素,而刺激跟踪是由杆和锥输入介导的。最后,行为分析表明,尽管所有三个感光系统对于对比度敏感度几乎同等重要,但只有视锥细胞和视杆对空间敏锐度有贡献。

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