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SVOP是一种进化上保守的突触小泡蛋白,提示了突触小泡的新转运功能。

SVOP, an evolutionarily conserved synaptic vesicle protein, suggests novel transport functions of synaptic vesicles.

作者信息

Janz R, Hofmann K, Südhof T C

机构信息

Center for Basic Neuroscience, Department of Molecular Genetics and Howard Hughes Medical Institute, The University of Texas Southwestern Medical School, Dallas, Texas 75235, USA.

出版信息

J Neurosci. 1998 Nov 15;18(22):9269-81. doi: 10.1523/JNEUROSCI.18-22-09269.1998.

Abstract

We describe a novel synaptic vesicle protein called SVOP that is distantly related to the synaptic vesicle proteins SV2A, SV2B, and SV2C (20-22% sequence identity). Both SVOP and SV2 contain 12 transmembrane regions. However, SV2 is highly glycosylated, whereas SVOP is not. Databank searches revealed that closely related homologs of SVOP are present in Caenorhabditis elegans and Drosophila (48% sequence identity), suggesting that SVOP is evolutionarily ancient. In contrast, no invertebrate orthologs of SV2 were detected. The sequences of SVOP and SV2 exhibit homology with transport proteins, in particular with mammalian organic cation and anion transporters. SVOP and SV2 are more distantly related to eukaryotic and bacterial phosphate, sugar, and organic acid transporters. SVOP is expressed at detectable levels only in brain and endocrine cells where it is primarily localized to synaptic vesicles and microvesicles. SVOP is present in all brain regions, with particularly high levels in large pyramidal neurons of the cerebral cortex. Immunocytochemical staining of adjacent rat brain sections for SVOP and SV2 demonstrated that SVOP and SV2 are probably coexpressed in most neurons. Although the functions of SV2 and SVOP remain obscure, the evolutionary conservation of SVOP, its hydrophobic nature, and its homology to transporters strongly support a role in the uptake of a novel, as yet unidentified component of synaptic vesicles. Thus synaptic vesicles contain two classes of abundant proteins with 12 transmembrane regions that are related to transporters, nonglycosylated SVOP and highly glycosylated SV2, suggesting that the transport functions of synaptic vesicles may be more complex than currently envisioned.

摘要

我们描述了一种名为SVOP的新型突触囊泡蛋白,它与突触囊泡蛋白SV2A、SV2B和SV2C有较远的亲缘关系(序列同一性为20 - 22%)。SVOP和SV2都含有12个跨膜区域。然而,SV2高度糖基化,而SVOP则不然。数据库搜索显示,秀丽隐杆线虫和果蝇中存在与SVOP密切相关的同源物(序列同一性为48%),这表明SVOP在进化上很古老。相比之下,未检测到SV2的无脊椎动物直系同源物。SVOP和SV2的序列与转运蛋白具有同源性,特别是与哺乳动物的有机阳离子和阴离子转运蛋白。SVOP和SV2与真核生物和细菌的磷酸盐、糖和有机酸转运蛋白的关系更远。SVOP仅在脑和内分泌细胞中以可检测的水平表达,主要定位于突触囊泡和微囊泡。SVOP存在于所有脑区,在大脑皮层的大型锥体神经元中含量特别高。对相邻大鼠脑切片进行的SVOP和SV2免疫细胞化学染色表明,SVOP和SV2可能在大多数神经元中共表达。尽管SV2和SVOP的功能仍不清楚,但SVOP的进化保守性、其疏水性以及与转运蛋白的同源性强烈支持其在摄取一种新的、尚未确定的突触囊泡成分中的作用。因此,突触囊泡含有两类丰富的具有12个跨膜区域且与转运蛋白相关的蛋白质,即非糖基化的SVOP和高度糖基化的SV2,这表明突触囊泡的转运功能可能比目前设想的更为复杂。

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