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γ-氨基丁酸能和甘氨酸能突触终末小体中囊泡抑制性氨基酸转运体的存在。

Presence of the vesicular inhibitory amino acid transporter in GABAergic and glycinergic synaptic terminal boutons.

作者信息

Dumoulin A, Rostaing P, Bedet C, Lévi S, Isambert M F, Henry J P, Triller A, Gasnier B

机构信息

Laboratoire de Biologie Cellulaire de la Synapse (INSERM U 497), Ecole Normale Supérieure, France.

出版信息

J Cell Sci. 1999 Mar;112 ( Pt 6):811-23. doi: 10.1242/jcs.112.6.811.

Abstract

The characterization of the Caenorhabditis elegans unc-47 gene recently allowed the identification of a mammalian (gamma)-amino butyric acid (GABA) transporter, presumed to be located in the synaptic vesicle membrane. In situ hybridization data in rat brain suggested that it might also take up glycine and thus represent a general Vesicular Inhibitory Amino Acid Transporter (VIAAT). In the present study, we have investigated the localization of VIAAT in neurons by using a polyclonal antibody raised against the hydrophilic N-terminal domain of the protein. Light microscopy and immunocytochemistry in primary cultures or tissue sections of the rat spinal cord revealed that VIAAT was localized in a subset (63-65%) of synaptophysin-immunoreactive terminal boutons; among the VIAAT-positive terminals around motoneuronal somata, 32.9% of them were also immunoreactive for GAD65, a marker of GABAergic presynaptic endings. Labelling was also found apposed to clusters positive for the glycine receptor or for its associated protein gephyrin. At the ultrastructural level, VIAAT immunoreactivity was restricted to presynaptic boutons exhibiting classical inhibitory features and, within the boutons, concentrated over synaptic vesicle clusters. Pre-embedding detection of VIAAT followed by post-embedding detection of GABA or glycine on serial sections of the spinal cord or cerebellar cortex indicated that VIAAT was present in glycine-, GABA- or GABA- and glycine-containing boutons. Taken together, these data further support the view of a common vesicular transporter for these two inhibitory transmitters, which would be responsible for their costorage in the same synaptic vesicle and subsequent corelease at mixed GABA-and-glycine synapses.

摘要

秀丽隐杆线虫unc-47基因的特性研究最近使得一种哺乳动物γ-氨基丁酸(GABA)转运体得以鉴定,该转运体被推测位于突触小泡膜上。大鼠脑内的原位杂交数据表明,它可能还摄取甘氨酸,因此代表一种通用的囊泡抑制性氨基酸转运体(VIAAT)。在本研究中,我们使用针对该蛋白亲水性N端结构域产生的多克隆抗体,研究了VIAAT在神经元中的定位。大鼠脊髓原代培养物或组织切片的光学显微镜和免疫细胞化学研究显示,VIAAT定位于突触素免疫反应性终末小体的一个亚群(63 - 65%)中;在运动神经元胞体周围的VIAAT阳性终末中,其中32.9%对GAD65也呈免疫反应性,GAD65是GABA能突触前末梢的标志物。还发现标记物与甘氨酸受体或其相关蛋白gephyrin阳性的簇相邻。在超微结构水平上,VIAAT免疫反应性仅限于呈现经典抑制特征的突触前小体,并且在小体内,集中于突触小泡簇上。在脊髓或小脑皮质的连续切片上,先进行VIAAT的包埋前检测,然后进行GABA或甘氨酸的包埋后检测,结果表明VIAAT存在于含甘氨酸、GABA或同时含GABA和甘氨酸的小体中。综上所述,这些数据进一步支持了这两种抑制性递质存在共同囊泡转运体的观点,该转运体负责它们在同一突触小泡中的共储存以及随后在混合GABA - 甘氨酸突触处的共同释放。

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