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2
Distinctive synaptic structural motifs link excitatory retinal interneurons to diverse postsynaptic partner types.特有的突触结构基元将兴奋性视网膜中间神经元与不同的突触后伙伴类型联系起来。
Cell Rep. 2023 Jan 31;42(1):112006. doi: 10.1016/j.celrep.2023.112006. Epub 2023 Jan 19.
3
Spatiotemporal properties of glutamate input support direction selectivity in the dendrites of retinal starburst amacrine cells.谷氨酸输入的时空特性支持视网膜星爆型无长突细胞树突的方向选择性。
Elife. 2022 Nov 8;11:e81533. doi: 10.7554/eLife.81533.
4
Classical center-surround receptive fields facilitate novel object detection in retinal bipolar cells.经典中心-环绕感受野促进视网膜双极细胞对新物体的检测。
Nat Commun. 2022 Sep 26;13(1):5575. doi: 10.1038/s41467-022-32761-8.
5
Center-surround interactions underlie bipolar cell motion sensitivity in the mouse retina.中心-环绕相互作用是小鼠视网膜双极细胞运动敏感性的基础。
Nat Commun. 2022 Sep 26;13(1):5574. doi: 10.1038/s41467-022-32762-7.
6
Orientation and direction tuning align with dendritic morphology and spatial connectivity in mouse visual cortex.方位和方向调谐与小鼠视觉皮层中的树突形态和空间连接一致。
Curr Biol. 2022 Apr 25;32(8):1743-1753.e7. doi: 10.1016/j.cub.2022.02.048. Epub 2022 Mar 10.
7
The influence of spontaneous and visual activity on the development of direction selectivity maps in mouse retina.自发性和视觉活动对小鼠视网膜方向选择性图谱发育的影响。
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Cholinergic feedback to bipolar cells contributes to motion detection in the mouse retina.胆碱能反馈对双极细胞的贡献有助于小鼠视网膜的运动检测。
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视网膜中多特征提取的神经回路。

Neural Circuits Underlying Multifeature Extraction in the Retina.

机构信息

Department of Biology, University of Victoria, Victoria, British Columbia V8W 4A4, Canada.

Department of Biology, University of Victoria, Victoria, British Columbia V8W 4A4, Canada

出版信息

J Neurosci. 2024 Mar 6;44(10):e0910232023. doi: 10.1523/JNEUROSCI.0910-23.2023.

DOI:10.1523/JNEUROSCI.0910-23.2023
PMID:37957014
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC10919202/
Abstract

Classic ON-OFF direction-selective ganglion cells (DSGCs) that encode the four cardinal directions were recently shown to also be orientation-selective. To clarify the mechanisms underlying orientation selectivity, we employed a variety of electrophysiological, optogenetic, and gene knock-out strategies to test the relative contributions of glutamate, GABA, and acetylcholine (ACh) input that are known to drive DSGCs, in male and female mouse retinas. Extracellular spike recordings revealed that DSGCs respond preferentially to either vertical or horizontal bars, those that are perpendicular to their preferred-null motion axes. By contrast, the glutamate input to all four DSGC types measured using whole-cell patch-clamp techniques was found to be tuned along the vertical axis. Tuned glutamatergic excitation was heavily reliant on type 5A bipolar cells, which appear to be electrically coupled via connexin 36 containing gap junctions to the vertically oriented processes of wide-field amacrine cells. Vertically tuned inputs are transformed by the GABAergic/cholinergic "starburst" amacrine cells (SACs), which are critical components of the direction-selective circuit, into distinct patterns of inhibition and excitation. Feed-forward SAC inhibition appears to "veto" preferred orientation glutamate excitation in dorsal/ventral (but not nasal/temporal) coding DSGCs "flipping" their orientation tuning by 90° and accounts for the apparent mismatch between glutamate input tuning and the DSGC's spiking response. Together, these results reveal how two distinct synaptic motifs interact to generate complex feature selectivity, shedding light on the intricate circuitry that underlies visual processing in the retina.

摘要

最近发现,经典的 ON-OFF 方向选择性神经节细胞(DSGC)不仅具有方向选择性,还能编码四个基本方向。为了阐明方向选择性的机制,我们采用了多种电生理、光遗传学和基因敲除策略,以测试已知驱动 DSGC 的谷氨酸、GABA 和乙酰胆碱(ACh)输入的相对贡献,这些输入在雄性和雌性小鼠视网膜中。细胞外尖峰记录显示,DSGC 优先对垂直或水平条带做出反应,这些条带与它们的首选-零运动轴垂直。相比之下,使用全细胞贴附式膜片钳技术测量的所有四种 DSGC 类型的谷氨酸输入被发现沿着垂直轴进行调谐。调谐的谷氨酸兴奋性强烈依赖于类型 5A 双极细胞,这些细胞似乎通过含有缝隙连接蛋白 36 的连接蛋白相互电耦合,与宽场无长突细胞的垂直方向过程相连。垂直调谐的输入被 GABA 能/胆碱能“星爆”无长突细胞(SAC)转化为抑制和兴奋的独特模式,SAC 是方向选择性电路的关键组成部分。前馈 SAC 抑制似乎“否决”了背/腹(但不是鼻/颞)编码 DSGC 中优先方向谷氨酸兴奋,通过 90°翻转其方向调谐,并解释了谷氨酸输入调谐与 DSGC 尖峰反应之间的明显不匹配。这些结果共同揭示了两种不同的突触模式如何相互作用产生复杂的特征选择性,为视网膜中视觉处理的复杂电路提供了线索。