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小鼠视网膜中囊泡相关膜蛋白亚型的差异分布。

Differential distribution of vesicle associated membrane protein isoforms in the mouse retina.

作者信息

Sherry David M, Wang Meng M, Frishman Laura J

机构信息

College of Optometry, University of Houston, Houston, TX 77204-2020, USA.

出版信息

Mol Vis. 2003 Dec 11;9:673-88.

Abstract

PURPOSE

Many proteins associated with synaptic vesicle exocytosis are differentially distributed among synapses in the retina and elsewhere in the central nervous system. The synapse-specific distribution of these proteins and their isoforms is thought to contribute to synapse-specific functional differences. Vesicle-associated membrane protein (VAMP, also known as synaptobrevin) is an integral synaptic vesicle membrane protein that is part of the fusion core complex needed for docking and fusing of synaptic vesicles at the synaptic active zone. Two VAMP isoforms have been identified that are considered to be synaptic, VAMP-1 and VAMP-2, however their distributions among the various synapses in the mammalian retina have not been characterized.

METHODS

Single- and double-labeling immunocytochemistry was used to investigate the distribution of the synaptic VAMP isoforms, VAMP-1 and VAMP-2, in the mouse retina.

RESULTS

VAMP-2 was the predominant isoform in both synaptic layers. Double-labeling studies using conventional and ribbon-synapse-specific markers showed that VAMP-2 was broadly distributed among conventional and ribbon synapses. In contrast, the distribution of VAMP-1 was very limited. In the outer retina, only weak labeling was present in photoreceptor terminals. In the inner retina, labeling for VAMP-1 was found in the dendrites, cell bodies, and axons of some ganglion cells, as demonstrated by double labeling with the ganglion cell markers, microtubule-associated protein-1 and Brn-3a. VAMP-1 labeling did not colocalize with amacrine or bipolar cell markers, nor did it colocalize with other pre-synaptic markers, suggesting that VAMP-1 is not associated directly with neurotransmitter release in the inner retina. Labeling for VAMP-1 identified a set of large ganglion cells that ramified in the mid-IPL (inner plexiform layer), suggesting that they may show ON-OFF responses. Some of these cells had cell bodies displaced to the inner nuclear layer. The dendrites of the large VAMP-1-immunoreactive ganglion cells did not co-stratify with the cholinergic plexuses of the starburst amacrine cells (labeled for choline acetyltransferase) and therefore are unlikely to show directional selectivity. However, these cells are likely to receive input from bipolar cells and a population of putative glutamatergic amacrine cells.

CONCLUSIONS

VAMP-1 and VAMP-2 are differentially distributed among the synapses of the mouse retina. VAMP-2 is the predominant isoform and is widely expressed at ribbon and conventional synapses in both plexiform layers. VAMP-1 expression in the mouse retina is much more limited and is not restricted to presynaptic terminals. In the OPL, VAMP-1 is co-expressed with VAMP-2 presynaptically in photoreceptor terminals. However, VAMP-1 expression in the IPL is associated with ganglion cells and does not appear to be localized to presynaptic terminals. VAMP-1 is a specific marker for a set of large ganglion cells and displaced ganglion cells that ramify in the mid-IPL and are likely to have ON-OFF physiology.

摘要

目的

许多与突触小泡胞吐作用相关的蛋白质在视网膜及中枢神经系统其他部位的突触间呈差异分布。这些蛋白质及其亚型的突触特异性分布被认为导致了突触特异性功能差异。囊泡相关膜蛋白(VAMP,也称为突触结合蛋白)是一种整合于突触小泡膜的蛋白质,是突触小泡在突触活性区对接和融合所需的融合核心复合体的一部分。已鉴定出两种被认为是突触性的VAMP亚型,即VAMP-1和VAMP-2,但它们在哺乳动物视网膜不同突触间的分布尚未明确。

方法

采用单标记和双标记免疫细胞化学方法研究突触VAMP亚型VAMP-1和VAMP-2在小鼠视网膜中的分布。

结果

VAMP-2是两个突触层中的主要亚型。使用传统和带状突触特异性标记物的双标记研究表明,VAMP-2广泛分布于传统突触和带状突触中。相比之下,VAMP-1的分布非常有限。在视网膜外层,仅在光感受器终末有微弱标记。在内层视网膜中,用神经节细胞标记物微管相关蛋白-1和Brn-3a进行双标记显示,在一些神经节细胞的树突、胞体和轴突中发现了VAMP-1标记。VAMP-1标记与无长突细胞或双极细胞标记物不共定位,也与其他突触前标记物不共定位,这表明VAMP-1在内层视网膜中不直接参与神经递质释放。VAMP-1标记鉴定出一组在中间内网状层(IPL)分支的大型神经节细胞,提示它们可能具有开-关反应。其中一些细胞的胞体移位至内核层。大型VAMP-1免疫反应性神经节细胞的树突不与星爆无长突细胞(用胆碱乙酰转移酶标记)的胆碱能丛共分层,因此不太可能表现出方向选择性。然而,这些细胞可能接受双极细胞和一群假定的谷氨酸能无长突细胞的输入。

结论

VAMP-1和VAMP-2在小鼠视网膜突触间呈差异分布。VAMP-2是主要亚型,在两个网状层的带状突触和传统突触中广泛表达。VAMP-1在小鼠视网膜中的表达更为有限,且不限于突触前终末。在视网膜外网状层(OPL),VAMP-1在光感受器终末与VAMP-2在突触前共同表达。然而,VAMP-1在IPL中的表达与神经节细胞相关,似乎并不局限于突触前终末。VAMP-1是一组在中间IPL分支且可能具有开-关生理特性的大型神经节细胞和移位神经节细胞的特异性标记物。

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