首页> 外文期刊>Journal of Neurochemistry: Offical Journal of the International Society for Neurochemistry >Targeted disruption of Sept3, a heteromeric assembly partner of Sept5 and Sept7 in axons, has no effect on developing CNS neurons.
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Targeted disruption of Sept3, a heteromeric assembly partner of Sept5 and Sept7 in axons, has no effect on developing CNS neurons.

机译:轴突中Sept5和Sept7的异源组装伴侣Sept3的靶向破坏对中枢神经系统神经元的发育没有影响。

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摘要

The septins constitute a family of GTPase proteins that are involved in many cytological processes such as cytokinesis and exocytosis. Previous studies have indicated that mammalian Sept3 is a brain-specific protein that is abundant in synaptic terminals. Here, we further investigated the localization and function of Sept3 in the mouse brain. Sept3 is expressed in several types of post-mitotic neurons, including granule cells in the cerebellum and pyramidal neurons in the cerebral cortex and hippocampus. In primary cultures of hippocampal pyramidal neurons, Sept3 protein is enriched at the tips of growing neurites during differentiation. Sept3 directly binds to Sept5 and Sept7 and forms a heteromeric complex at nerve terminals adjacent to where a synaptic vesicle marker, synaptophysin, is expressed in mature neurons. When over-expressed in HEK293 cells, Sept3 forms filamentous structures that are dependent on the presence of its GTP- and phosphoinositide-binding domains. To investigate the physiological roles of Sept3, we generated Sept3 deficient mice. These mice show no apparent abnormalities in histogenesis nor neuronal differentiation in culture. Expression of synaptic proteins and other septins are unaltered, indicating that Sept3 is dispensable for normal neuronal development.
机译:隔离蛋白构成GTPase蛋白家族,涉及许多细胞学过程,例如胞质分裂和胞吐作用。先前的研究表明,哺乳动物Sept3是一种大脑特异性蛋白,在突触末端丰富。在这里,我们进一步研究了Sept3在小鼠脑中的定位和功能。 Sept3在几种类型的有丝分裂后神经元中表达,包括小脑中的颗粒细胞和大脑皮质和海马中的锥体神经元。在海马锥体神经元的原代培养中,Sept3蛋白在分化过程中生长的神经突尖端富集。 Sept3直接与Sept5和Sept7结合,并在神经末梢形成异源复合物,该末端与成熟神经元中表达突触囊泡标记突触素的位置相邻。当在HEK293细胞中过表达时,Sept3会形成丝状结构,这取决于其GTP和磷酸肌醇结合域的存在。为了调查Sept3的生理作用,我们生成了Sept3缺陷小鼠。这些小鼠在组织发生或培养中神经元分化方面均未显示明显异常。突触蛋白和其他septins的表达未改变,表明Sept3对于正常的神经元发育是可有可无的。

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