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Intersectin调节海马神经元中树突棘的发育和体树突内吞作用,但不调节突触小泡循环。

Intersectin regulates dendritic spine development and somatodendritic endocytosis but not synaptic vesicle recycling in hippocampal neurons.

作者信息

Thomas Sébastien, Ritter Brigitte, Verbich David, Sanson Claire, Bourbonnière Lyne, McKinney R Anne, McPherson Peter S

机构信息

Department of Neurology and Neurosurgery, Montreal Neurological Institute, McGill University, Montreal, Quebec H3A 2B4, Canada.

出版信息

J Biol Chem. 2009 May 1;284(18):12410-9. doi: 10.1074/jbc.M809746200. Epub 2009 Mar 3.

Abstract

Intersectin-short (intersectin-s) is a multimodule scaffolding protein functioning in constitutive and regulated forms of endocytosis in non-neuronal cells and in synaptic vesicle (SV) recycling at the neuromuscular junction of Drosophila and Caenorhabditis elegans. In vertebrates, alternative splicing generates a second isoform, intersectin-long (intersectin-l), that contains additional modular domains providing a guanine nucleotide exchange factor activity for Cdc42. In mammals, intersectin-s is expressed in multiple tissues and cells, including glia, but excluded from neurons, whereas intersectin-l is a neuron-specific isoform. Thus, intersectin-I may regulate multiple forms of endocytosis in mammalian neurons, including SV endocytosis. We now report, however, that intersectin-l is localized to somatodendritic regions of cultured hippocampal neurons, with some juxtanuclear accumulation, but is excluded from synaptophysin-labeled axon terminals. Consistently, intersectin-l knockdown (KD) does not affect SV recycling. Instead intersectin-l co-localizes with clathrin heavy chain and adaptor protein 2 in the somatodendritic region of neurons, and its KD reduces the rate of transferrin endocytosis. The protein also co-localizes with F-actin at dendritic spines, and intersectin-l KD disrupts spine maturation during development. Our data indicate that intersectin-l is indeed an important regulator of constitutive endocytosis and neuronal development but that it is not a prominent player in the regulated endocytosis of SVs.

摘要

截短型Intersectin(Intersectin-s)是一种多模块支架蛋白,在非神经元细胞的组成型和调节型内吞作用以及果蝇和秀丽隐杆线虫神经肌肉接头处的突触小泡(SV)循环中发挥作用。在脊椎动物中,可变剪接产生了第二种异构体,即长型Intersectin(Intersectin-l),它包含额外的模块化结构域,为Cdc42提供鸟嘌呤核苷酸交换因子活性。在哺乳动物中,Intersectin-s在包括神经胶质细胞在内的多种组织和细胞中表达,但在神经元中不表达,而Intersectin-l是神经元特异性异构体。因此,Intersectin-l可能调节哺乳动物神经元内吞作用的多种形式,包括SV内吞作用。然而,我们现在报告,Intersectin-l定位于培养的海马神经元的树突状区域,有一些核周积累,但在突触素标记的轴突终末中不存在。一致地,Intersectin-l基因敲低(KD)不影响SV循环。相反,Intersectin-l在神经元的树突状区域与网格蛋白重链和衔接蛋白2共定位,其KD降低了转铁蛋白内吞作用的速率。该蛋白在树突棘处也与F-肌动蛋白共定位,Intersectin-l KD在发育过程中破坏了棘的成熟。我们的数据表明,Intersectin-l确实是组成型内吞作用和神经元发育的重要调节因子,但它在SV的调节型内吞作用中不是主要参与者。

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