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大鼠中枢神经系统中突触结合蛋白I、II、III和IV mRNA的发育调控

Developmental regulation of synaptotagmin I, II, III, and IV mRNAs in the rat CNS.

作者信息

Berton F, Iborra C, Boudier J A, Seagar M J, Marquèze B

机构信息

Institut National de la Santé et de la Recherche Médicale U 374, Institut Jean Roche, Faculté de Médecine-Secteur Nord, 13916 Marseille Cedex 20, France.

出版信息

J Neurosci. 1997 Feb 15;17(4):1206-16. doi: 10.1523/JNEUROSCI.17-04-01206.1997.

Abstract

Synaptotagmin I is an abundant synaptic vesicle protein that has an essential function in mediating Ca2+-triggered neurotransmitter release. We have analyzed the distribution of four neural synaptotagmin isoforms during postnatal development of the rat CNS by in situ hybridization. Synaptotagmin I, II, III, and IV genes have distinct patterns of spatiotemporal expression except in cerebellum granule cells, where the four transcripts were detected during the formation of parallel fiber/Purkinje cell synapses. Throughout development synaptotagmin I mRNAs were widely expressed in brain, whereas synaptotagmin II transcripts were predominant in spinal cord. At all stages synaptotagmin III mRNAs were expressed uniformly in most neurons examined, although at a low level. Synaptotagmin I, II, and III gene expressions mainly increased during development and persisted in adulthood, mirroring neuronal differentiation. Conversely, synaptotagmin IV transcripts were predominant during perinatal development in a heterogeneous population of neurons and subsequently were expressed uniformly at a low level. Intense labeling was observed in the hippocampal CA3 field and in the subiculum, but not in the CA1 field, of the newborn rat. In cerebral cortex, lamina-specific labeling was detected with a high expression in cell layer V. Only a small number of Purkinje cell clusters were labeled in the flocculus and paraflocculus of the cerebellum. Heterogeneous sets of neurons expressing synaptotagmin IV gene also were observed in spinal cord. We thus speculate that synaptotagmin IV may a play a role in the development of the mammalian nervous system.

摘要

突触结合蛋白I是一种丰富的突触囊泡蛋白,在介导Ca2+触发的神经递质释放中具有重要作用。我们通过原位杂交分析了大鼠中枢神经系统出生后发育过程中四种神经突触结合蛋白亚型的分布。突触结合蛋白I、II、III和IV基因具有不同的时空表达模式,但在小脑颗粒细胞中除外,在平行纤维/浦肯野细胞突触形成过程中可检测到这四种转录本。在整个发育过程中,突触结合蛋白I的mRNA在脑中广泛表达,而突触结合蛋白II的转录本在脊髓中占主导。在所有阶段,突触结合蛋白III的mRNA在大多数检测的神经元中均有均匀表达,尽管水平较低。突触结合蛋白I、II和III的基因表达在发育过程中主要增加,并在成年期持续存在,反映了神经元的分化。相反,突触结合蛋白IV的转录本在围产期发育期间在异质神经元群体中占主导,随后以低水平均匀表达。在新生大鼠的海马CA3区和下托中观察到强烈标记,但在CA1区未观察到。在大脑皮层中,检测到层特异性标记,在V层细胞中有高表达。在小脑的绒球和旁绒球中仅标记了少数浦肯野细胞簇。在脊髓中也观察到表达突触结合蛋白IV基因的异质神经元组。因此,我们推测突触结合蛋白IV可能在哺乳动物神经系统的发育中起作用。

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