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Shared and distinct retinal input to the mouse superior colliculus and dorsal lateral geniculate nucleus

机译:共享的和不同的视网膜输入到小鼠上丘和背外侧膝状核

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摘要

The mammalian retina conveys the vast majority of information about visual stimuli to two brain regions: the dorsal lateral geniculate nucleus (dLGN) and the superior colliculus (SC). The degree to which retinal ganglion cells (RGCs) send similar or distinct information to the two areas remains unclear despite the important constraints that different patterns of RGC input place on downstream visual processing. To resolve this ambiguity, we injected a glycoprotein-deficient rabies virus coding for the expression of a fluorescent protein into the dLGN or SC; rabies virus labeled a smaller fraction of RGCs than lipophilic dyes such as DiI but, crucially, did not label RGC axons of passage. Approximately 80% of the RGCs infected by rabies virus injected into the dLGN were colabeled with DiI injected into the SC, suggesting that many dLGN-projecting RGCs also project to the SC. However, functional characterization of RGCs revealed that the SC receives input from several classes of RGCs that largely avoid the dLGN, in particular RGCs in which 1) sustained changes in light intensity elicit transient changes in firing rate and/or 2) a small range of stimulus sizes or temporal fluctuations in light intensity elicit robust activity. Taken together, our results illustrate several unexpected asymmetries in the information that the mouse retina conveys to two major downstream targets and suggest that differences in the output of dLGN and SC neurons reflect, at least in part, differences in the functional properties of RGCs that innervate the SC but not the dLGN.
机译:哺乳动物的视网膜将有关视觉刺激的绝大多数信息传递到两个大脑区域:背外侧膝状核(dLGN)和上丘(SC)。尽管RGC输入的不同模式对下游视觉处理产生了重要限制,但视网膜神经节细胞(RGC)向两个区域发送相似或不同信息的程度仍不清楚。为了解决这种歧义,我们将编码荧光蛋白表达的糖蛋白缺陷型狂犬病毒注射到dLGN或SC中。狂犬病毒标记的RGC的比例比亲脂性染料(如DiI)小,但至关重要的是,并未标记RGC轴突的通过。注射到dLGN中的狂犬病病毒感染的RGC大约有80%与注入SC的DiI共同标记,表明许多投射dLGN的RGC也投射到SC。但是,RGC的功能特性表明,SC从几类RGC接收了输入,这些RGC在很大程度上避免了dLGN,特别是其中1)光强度的持续变化引起发射速率的瞬态变化和/或2)很小范围的RGC。刺激大小或光强度的时间波动会引起强烈的活动。两者合计,我们的结果说明了鼠标视网膜传递给两个主要下游靶标的信息中出现了一些意外的不对称现象,并表明dLGN和SC神经元输出的差异至少部分反映了神经支配的RGC功能特性的差异。 SC,但不是dLGN。

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