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Photoresponse diversity among the five types of intrinsically photosensitive retinal ganglion cells

机译:五种固有光敏性视网膜神经节细胞之间的光响应多样性

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摘要

Intrinsically photosensitive retinal ganglion cells (ipRGCs) mediate non-image-forming visual responses, including pupillary constriction, circadian photoentrainment and suppression of pineal melatonin secretion. Five morphological types of ipRGCs, M1–M5, have been identified in mice. In order to understand their functions better, we studied the photoresponses of all five cell types, by whole-cell recording from fluorescently labelled ipRGCs visualized using multiphoton microscopy. All ipRGC types generated melanopsin-based (‘intrinsic’) as well as synaptically driven (‘extrinsic’) light responses. The intrinsic photoresponses of M1 cells were lower threshold, higher amplitude and faster than those of M2–M5. The peak amplitudes of extrinsic light responses differed among the ipRGC types; however, the responses of all cell types had comparable thresholds, kinetics and waveforms, and all cells received rod input. While all five types exhibited inhibitory amacrine-cell and excitatory bipolar-cell inputs from the ‘on’ channel, M1 and M3 received additional ‘off’-channel inhibition, possibly through their ‘off’-sublamina dendrites. The M2–M5 ipRGCs had centre–surround-organized receptive fields, implicating a capacity to detect spatial contrast. In contrast, the receptive fields of M1 cells lacked surround antagonism, which might be caused by the surround of the inhibitory input nullifying the surround of the excitatory input. All ipRGCs responded robustly to a wide range of motion speeds, and M1–M4 cells appeared tuned to different speeds, suggesting that they might analyse the speed of motion. Retrograde labelling revealed that M1–M4 cells project to the superior colliculus, suggesting that the contrast and motion information signalled by these cells could be used by this sensorimotor area to detect novel objects and motion in the visual field.
机译:本质上光敏性视网膜神经节细胞(ipRGCs)介导非图像形成的视觉反应,包括瞳孔收缩,昼夜节律性光吸收和松果体褪黑激素分泌的抑制。已在小鼠中鉴定出五种形态类型的ipRGC,即M1-M5。为了更好地了解它们的功能,我们通过使用多光子显微镜观察的荧光标记ipRGC的全细胞记录研究了所有五种细胞类型的光响应。所有ipRGC类型都产生基于黑素的(“本征”)以及突触驱动的(“本征”)光响应。 M1细胞的固有光响应比M2-M5的阈值低,幅度高,速度快。外部光响应的峰值幅度在ipRGC类型之间有所不同。但是,所有细胞类型的响应具有可比的阈值,动力学和波形,并且所有细胞都接受了杆输入。尽管所有五种类型均显示来自“ on”通道的抑制性无长分泌细胞和兴奋性双极细胞输入,但M1和M3可能通过其“ off”-亚层突状树突接受了额外的“ off”-通道抑制。 M2-M5 ipRGC具有中心-周围组织的接收场,暗示了检测空间对比度的能力。相反,M1细胞的感受野缺乏周围拮抗作用,这可能是由于抑制性输入的周围使兴奋性输入的周围无效而引起的。所有ipRGC对多种运动速度都有很强的响应能力,M1-M4细胞似乎已调节到不同的速度,这表明它们可以分析运动速度。逆行标记显示M1–M4细胞投射到上丘,提示这些细胞发出的对比度和运动信息可被该感觉运动区域用来检测视野中的新物体和运动。

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