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海马神经元中异聚体γ-氨基丁酸B型受体亚基的树突状组装

Dendritic assembly of heteromeric gamma-aminobutyric acid type B receptor subunits in hippocampal neurons.

作者信息

Ramírez Omar A, Vidal René L, Tello Judith A, Vargas Karina J, Kindler Stefan, Härtel Steffen, Couve Andrés

机构信息

Physiology and Biophysics, Faculty of Medicine, Universidad de Chile, Santiago, Chile.

出版信息

J Biol Chem. 2009 May 8;284(19):13077-85. doi: 10.1074/jbc.M900575200. Epub 2009 Mar 10.

Abstract

Understanding the mechanisms that control synaptic efficacy through the availability of neurotransmitter receptors depends on uncovering their specific intracellular trafficking routes. gamma-Aminobutyric acid type B (GABA(B)) receptors (GABA(B)Rs) are obligatory heteromers present at dendritic excitatory and inhibitory postsynaptic sites. It is unknown whether synthesis and assembly of GABA(B)Rs occur in the somatic endoplasmic reticulum (ER) followed by vesicular transport to dendrites or whether somatic synthesis is followed by independent transport of the subunits for assembly and ER export throughout the somatodendritic compartment. To discriminate between these possibilities we studied the association of GABA(B)R subunits in dendrites of hippocampal neurons combining live fluorescence microscopy, biochemistry, quantitative colocalization, and bimolecular fluorescent complementation. We demonstrate that GABA(B)R subunits are segregated and differentially mobile in dendritic intracellular compartments and that a high proportion of non-associated intracellular subunits exist in the brain. Assembled heteromers are preferentially located at the plasma membrane, but blockade of ER exit results in their intracellular accumulation in the cell body and dendrites. We propose that GABA(B)R subunits assemble in the ER and are exported from the ER throughout the neuron prior to insertion at the plasma membrane. Our results are consistent with a bulk flow of segregated subunits through the ER and rule out a post-Golgi vesicular transport of preassembled GABA(B)Rs.

摘要

通过神经递质受体的可用性来理解控制突触效能的机制,依赖于揭示其特定的细胞内运输途径。γ-氨基丁酸B型(GABA(B))受体(GABA(B)Rs)是存在于树突兴奋性和抑制性突触后位点的 obligatory 异聚体。目前尚不清楚GABA(B)Rs的合成和组装是在体细胞内质网(ER)中发生,随后通过囊泡运输到树突,还是体细胞合成之后,亚基独立运输以在整个树突状细胞区室进行组装和内质网输出。为了区分这些可能性,我们结合实时荧光显微镜、生物化学、定量共定位和双分子荧光互补技术,研究了海马神经元树突中GABA(B)R亚基的关联。我们证明,GABA(B)R亚基在树突细胞内区室中是分离的且具有不同的移动性,并且大脑中存在高比例的未关联细胞内亚基。组装好的异聚体优先位于质膜,但内质网输出的阻断会导致它们在细胞体和树突中细胞内积累。我们提出,GABA(B)R亚基在内质网中组装,并在插入质膜之前从内质网输出到整个神经元。我们的结果与分离的亚基通过内质网的大量流动一致,并排除了组装好的GABA(B)Rs的高尔基体后囊泡运输。

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