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突触微电路的连接组学:外视网膜的启示。

Connectomics of synaptic microcircuits: lessons from the outer retina.

机构信息

Institute for Ophthalmic Research, University of Tübingen, 72076, Tübingen, Germany.

Centre for Integrative Neuroscience, University of Tübingen, 72076, Tübingen, Germany.

出版信息

J Physiol. 2017 Aug 15;595(16):5517-5524. doi: 10.1113/JP273671. Epub 2017 May 4.

Abstract

Photoreceptors form a sophisticated synaptic complex with bipolar and horizontal cells, transmitting the signals generated by the phototransduction cascade to downstream retinal circuitry. The cone photoreceptor synapse shows several characteristic anatomical connectivity motifs that shape signal transfer: typically, ON-cone bipolar cells receive photoreceptor input through invaginating synapses; OFF-cone bipolar cells form basal synapses with photoreceptors. Both ON- and OFF-cone bipolar cells are believed to sample from all cone photoreceptors within their dendritic span. Electron microscopy and immunolabelling studies have established the robustness of these motifs, but have been limited by trade-offs in sample size and spatial resolution, respectively, constraining precise quantitative investigation to a few individual cells. 3D-serial electron microscopy overcomes these limitations and has permitted complete sets of neurons to be reconstructed over a comparatively large section of retinal tissue. Although the published mouse dataset lacks labels for synaptic structures, the characteristic anatomical motifs at the photoreceptor synapse can be exploited to identify putative synaptic contacts, which has enabled the development of a quantitative description of outer retinal connectivity. This revealed unexpected exceptions to classical motifs, including substantial interaction between rod and cone pathways at the photoreceptor synapse, sparse photoreceptor sampling and atypical contacts. Here, we summarize what was learned from this study in a more general context: we consider both the implications and limitations of the study and identify promising avenues for future research.

摘要

光感受器与双极细胞和水平细胞形成复杂的突触复合体,将光转导级联产生的信号传递到下游视网膜回路。圆锥光感受器突触显示出几种特征性的解剖连接模式,这些模式决定了信号的传递:通常,ON-圆锥双极细胞通过内陷突触接收光感受器的输入;OFF-圆锥双极细胞与光感受器形成基底突触。ON-和 OFF-圆锥双极细胞都被认为在其树突跨度内从所有圆锥光感受器中取样。电子显微镜和免疫标记研究已经证实了这些模式的稳健性,但分别受到样本大小和空间分辨率的权衡限制,限制了对少数个别细胞的精确定量研究。3D 连续电子显微镜克服了这些限制,可以对相对较大的视网膜组织部分进行完整的神经元重建。尽管已发表的小鼠数据集缺乏突触结构的标签,但在光感受器突触处的特征性解剖模式可用于识别潜在的突触接触,这使得对外视网膜连接进行定量描述成为可能。这揭示了经典模式的一些意外例外,包括光感受器突触处的杆状和锥状通路之间的大量相互作用、稀疏的光感受器取样和非典型接触。在这里,我们在更广泛的背景下总结了从这项研究中学到的东西:我们既考虑了这项研究的意义和局限性,也确定了未来研究的有前途的途径。

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