首页> 外文期刊>The Journal of Comparative Neurology >Functional allocation of synaptic contacts in microcircuits from rods via rod bipolar to AII amacrine cells in the mouse retina
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Functional allocation of synaptic contacts in microcircuits from rods via rod bipolar to AII amacrine cells in the mouse retina

机译:从杆经由双极杆到小鼠视网膜中的AII无长突细胞的微电路中突触接触的功能分配

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Retinal microcircuits for night vision at the absolute threshold are required to relay a single-photon rod signal reliably to ganglion cells via rod bipolar (RB) cells and AII amacrine cells. To assess the noise reduction of intercellular signal transmission in this rod-specific pathway, we quantified its synaptic connectivity by 3D reconstruction of a series of electron micrographs. In most cases (94%), each rod made ribbon synaptic contacts onto two adjacent RB cells. Conversely, each RB cell was contacted by 25 rods. Each RB axon terminal contacted four or five AII amacrine cells via 53 ribbon synapses. Thus, the signal from one rod may be represented as 106 replicates at two RB axons. Moreover, the two adjacent RB cells contacted two to four AII amacrine cells in common, where the signals relayed by two RB cells were reunited. In more detail, over 50% of each RB output was directed predominantly to a single, preferred AII amacrine cell, although each RB cell also separately contacted another one to three AII amacrine cells. Most of the replicate signals at two RB axons were collected on a few AII amacrine cells via reunions, dominant connections, and electrical coupling by AII-AII gap junctions. Thus the original signal may be reliably represented by signal amplification with focal accumulation without gathering unnecessary noise from a wide surrounding area. This allocation of RB-AII synaptic contacts may serve as the structural basis for the physiological properties of the AII single-photon response that include high amplification, local adaptation, and regenerative acceleration.
机译:要求在绝对阈值下进行夜视的视网膜微电路将单光子棒信号可靠地通过棒双极(RB)细胞和AII Amacrine细胞传递给神经节细胞。为了评估该杆特异性途径中细胞间信号传递的噪声降低,我们通过一系列电子显微照片的3D重建量化了其突触连接性。在大多数情况下(94%),每个杆都在两个相邻的RB细胞上进行带状突触接触。相反,每个RB细胞通过25条棒接触。每个RB轴突末端通过53条带状突触接触了四个或五个AII阿马克林细胞。因此,来自一个杆的信号可以表示为在两个RB轴突处的106个重复。此外,两个相邻的RB细胞共同接触2到4个AII阿马克林细胞,其中两个RB细胞中继的信号重新结合。更详细地讲,每个RB输出的50%以上主要针对单个优选的AII Amacrine细胞,尽管每个RB细胞也分别与另一到三个AII Amacrine细胞接触。在两个RB轴突处的大多数复制信号是通过团聚,主要连接和通过AII-AII间隙连接的电耦合收集在一些AII的无长突细胞上的。因此,可以通过具有焦点累积的信号放大来可靠地表示原始信号,而不会从宽广的周围区域收集不必要的噪声。 RB-AII突触接触的这种分配可以作为AII单光子响应的生理特性的结构基础,包括高扩增,局部适应和再生加速。

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