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突触素1的双磷酸酶活性对于神经末梢高效的突触囊泡内吞作用和再利用都是必需的。

The dual phosphatase activity of synaptojanin1 is required for both efficient synaptic vesicle endocytosis and reavailability at nerve terminals.

作者信息

Mani Meera, Lee Sang Yoon, Lucast Louise, Cremona Ottavio, Di Paolo Gilbert, De Camilli Pietro, Ryan Timothy A

机构信息

Department of Biochemistry, Weill Medical College of Cornell University, 1300 York Avenue, New York, NY 10021, USA.

出版信息

Neuron. 2007 Dec 20;56(6):1004-18. doi: 10.1016/j.neuron.2007.10.032.

Abstract

Phosphoinositides have been implicated in synaptic vesicle recycling largely based on studies of enzymes that regulate phosphoinositide synthesis and hydrolysis. One such enzyme is synaptojanin1, a multifunctional protein conserved from yeast to humans, which contains two phosphoinositol phosphatase domains and a proline-rich domain. Genetic ablation of synaptojanin1 leads to pleiotropic defects in presynaptic function, including accumulation of free clathrin-coated vesicles and delayed vesicle reavailability, implicating this enzyme in postendocytic uncoating of vesicles. To further elucidate the role of synaptojanin1 at nerve terminals, we performed quantitative synaptic vesicle recycling assays in synj1(-/-) neurons. Our studies show that synaptojanin1 is also required for normal vesicle endocytosis. Defects in both endocytosis and postendocytic vesicle reavailability can be fully restored upon reintroduction of synaptojanin1. However, expression of synaptojanin1 with mutations abolishing catalytic activity of each phosphatase domain reveals that the dual action of both domains is required for normal synaptic vesicle internalization and reavailability.

摘要

磷酸肌醇在突触小泡循环中的作用主要基于对调节磷酸肌醇合成和水解的酶的研究。其中一种酶是突触素1,它是一种从酵母到人类都保守的多功能蛋白,包含两个磷酸肌醇磷酸酶结构域和一个富含脯氨酸的结构域。突触素1的基因敲除导致突触前功能出现多效性缺陷,包括游离网格蛋白包被小泡的积累和小泡再利用的延迟,这表明该酶参与了小泡内吞后的脱包被过程。为了进一步阐明突触素1在神经末梢的作用,我们在synj1(-/-)神经元中进行了定量突触小泡循环测定。我们的研究表明,正常的小泡内吞作用也需要突触素1。重新引入突触素1后,内吞作用和内吞后小泡再利用的缺陷都可以完全恢复。然而,表达每个磷酸酶结构域催化活性被消除的突变型突触素1表明,两个结构域的双重作用对于正常的突触小泡内化和再利用是必需的。

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