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涉及多巴胺合成和运输到突触小泡的生化和功能蛋白复合物。

A biochemical and functional protein complex involving dopamine synthesis and transport into synaptic vesicles.

机构信息

Department of Neurobiology, University of Pittsburgh School of Medicine, Pittsburgh, PA 15261, USA.

出版信息

J Biol Chem. 2010 Jan 15;285(3):1957-66. doi: 10.1074/jbc.M109.054510. Epub 2009 Nov 10.

Abstract

Synaptic transmission depends on neurotransmitter pools stored within vesicles that undergo regulated exocytosis. In the brain, the vesicular monoamine transporter-2 (VMAT(2)) is responsible for the loading of dopamine (DA) and other monoamines into synaptic vesicles. Prior to storage within vesicles, DA synthesis occurs at the synaptic terminal in a two-step enzymatic process. First, the rate-limiting enzyme tyrosine hydroxylase (TH) converts tyrosine to di-OH-phenylalanine. Aromatic amino acid decarboxylase (AADC) then converts di-OH-phenylalanine into DA. Here, we provide evidence that VMAT(2) physically and functionally interacts with the enzymes responsible for DA synthesis. In rat striata, TH and AADC co-immunoprecipitate with VMAT(2), whereas in PC 12 cells, TH co-immunoprecipitates with the closely related VMAT(1) and with overexpressed VMAT(2). GST pull-down assays further identified three cytosolic domains of VMAT(2) involved in the interaction with TH and AADC. Furthermore, in vitro binding assays demonstrated that TH directly interacts with VMAT(2). Additionally, using fractionation and immunoisolation approaches, we demonstrate that TH and AADC associate with VMAT(2)-containing synaptic vesicles from rat brain. These vesicles exhibited specific TH activity. Finally, the coupling between synthesis and transport of DA into vesicles was impaired in the presence of fragments involved in the VMAT(2)/TH/AADC interaction. Taken together, our results indicate that DA synthesis can occur at the synaptic vesicle membrane, where it is physically and functionally coupled to VMAT(2)-mediated transport into vesicles.

摘要

突触传递依赖于储存在囊泡中的神经递质池,这些囊泡通过调节性胞吐作用释放神经递质。在大脑中,囊泡单胺转运体-2(VMAT(2))负责将多巴胺(DA)和其他单胺类物质装载到突触囊泡中。在囊泡内储存之前,DA 的合成发生在突触末端的两步酶促过程中。首先,限速酶酪氨酸羟化酶(TH)将酪氨酸转化为二羟苯丙氨酸。然后芳香族氨基酸脱羧酶(AADC)将二羟苯丙氨酸转化为 DA。在这里,我们提供了证据表明 VMAT(2) 与负责 DA 合成的酶在物理和功能上相互作用。在大鼠纹状体中,TH 和 AADC 与 VMAT(2) 共免疫沉淀,而在 PC12 细胞中,TH 与密切相关的 VMAT(1) 和过表达的 VMAT(2) 共免疫沉淀。GST 下拉实验进一步鉴定了 VMAT(2) 的三个胞质域,这些域参与与 TH 和 AADC 的相互作用。此外,体外结合实验表明 TH 直接与 VMAT(2) 相互作用。此外,通过分级分离和免疫隔离方法,我们证明 TH 和 AADC 与来自大鼠脑的含有 VMAT(2) 的突触囊泡相关联。这些囊泡表现出特定的 TH 活性。最后,在存在涉及 VMAT(2)/TH/AADC 相互作用的片段的情况下,DA 合成到囊泡中的合成和转运之间的偶联受到损害。总之,我们的结果表明,DA 的合成可以发生在突触囊泡膜上,在那里它与 VMAT(2) 介导的转运到囊泡中在物理和功能上偶联。

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