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小鼠视网膜中α神经节细胞的形态及示踪剂耦合模式

Morphology and tracer coupling pattern of alpha ganglion cells in the mouse retina.

作者信息

Völgyi Béla, Abrams Joseph, Paul David L, Bloomfield Stewart A

机构信息

Department of Ophthalmology, New York University School of Medicine, New York, New York 10016, USA.

出版信息

J Comp Neurol. 2005 Nov 7;492(1):66-77. doi: 10.1002/cne.20700.

Abstract

Alpha cells are a type of ganglion cell whose morphology appears to be conserved across a number of mammalian retinas. In particular, alpha cells display the largest somata and dendritic arbors at a given eccentricity and tile the retina as independent on- (ON) and off-center (OFF) subtypes. Mammalian alpha cells also express a variable tracer coupling pattern, which often includes homologous (same cell type) coupling to a few neighboring alpha cells and extensive heterologous (different cell type) coupling to two to three amacrine cell types. Here, we use the gap junction-permeant tracer Neurobiotin to determine the architecture and coupling pattern of alpha cells in the mouse retina. We find that alpha cells show the same somatic and dendritic architecture described previously in the mammal. However, alpha cells show varied tracer coupling patterns related to their ON and OFF physiologies. ON alpha cells show no evidence of homologous tracer coupling but are coupled heterologously to at least two types of amacrine cell whose somata lie within the ganglion cell layer. In contrast, OFF alpha cells are coupled to one another in circumscribed arrays as well as to two to three types of amacrine cell with somata occupying the inner nuclear layer. We find that homologous coupling between OFF alpha cells is unaltered in the connexin36 (Cx36) knockout (KO) mouse retina, indicating that it is not dependent on Cx36. However, a subset of the heterologous coupling of ON alpha cells and all the heterologous coupling of OFF alpha cells are eliminated in the KO retina, suggesting that Cx36 comprises most of the junctions made with amacrine cells.

摘要

α细胞是一种神经节细胞,其形态在多种哺乳动物视网膜中似乎是保守的。特别是,α细胞在给定的偏心度下呈现出最大的胞体和树突分支,并作为独立的ON(开)和OFF(关)亚型平铺在视网膜上。哺乳动物的α细胞还表现出可变的示踪剂耦合模式,通常包括与少数相邻α细胞的同源(相同细胞类型)耦合以及与两到三种无长突细胞类型的广泛异源(不同细胞类型)耦合。在这里,我们使用可透过缝隙连接的示踪剂神经生物素(Neurobiotin)来确定小鼠视网膜中α细胞的结构和耦合模式。我们发现α细胞呈现出与先前在哺乳动物中描述的相同的胞体和树突结构。然而,α细胞表现出与其ON和OFF生理功能相关的不同示踪剂耦合模式。ON型α细胞没有同源示踪剂耦合的证据,但与至少两种胞体位于神经节细胞层内的无长突细胞类型进行异源耦合。相比之下,OFF型α细胞在外围阵列中相互耦合,并且与两到三种胞体占据内核层的无长突细胞类型耦合。我们发现在连接蛋白36(Cx36)基因敲除(KO)小鼠视网膜中,OFF型α细胞之间的同源耦合没有改变,这表明它不依赖于Cx36。然而,ON型α细胞的一部分异源耦合以及OFF型α细胞的所有异源耦合在KO视网膜中被消除,这表明Cx36构成了与无长突细胞形成的大多数连接。

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