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蛋白质组学分析突触前活性区。

Proteomic analysis of the presynaptic active zone.

机构信息

Neurochemistry, Institute for Cell Biology and Neuroscience, Goethe University, Max-von-Laue-Str. 13, 60438 Frankfurt am Main, Germany.

出版信息

Exp Brain Res. 2012 Apr;217(3-4):449-61. doi: 10.1007/s00221-012-3031-x. Epub 2012 Feb 22.

Abstract

Synaptic vesicles are key organelles in chemical signaling, allowing neurons to communicate with each other and with neighboring cells. Vesicle integral or membrane-associated proteins mediate the various tasks the organelle fulfills during its life cycle. These include organelle transport, interaction with the nerve terminal cytoskeleton, uptake and storage of low molecular weight constituents, and the regulated interaction with the presynaptic plasma membrane, the active zone, during exo- and endocytosis. Converging work from several laboratories within the last 30 years resulted in the molecular and functional characterization of the protein inventory of the synaptic vesicle compartment. Nowadays advances in membrane protein separation and mass spectrometry have dramatically promoted this field resulting in a detailed description of the synaptic vesicle proteome and making synaptic vesicles the best characterized organelles. Recently, the proteome of the active zone was identified using the docked synaptic vesicles as target for immunoisolation. Combining gel-based protein separation techniques, mass spectrometry, and immunodetection, a considerable variety of proteins has been detected in the active zone. This includes synaptic vesicle proteins, components of the presynaptic fusion and retrieval machinery, proteins involved in intracellular signal transduction, a large variety of adhesion molecules and proteins potentially involved in regulating the functional and structural dynamics of the presynapse. Here, we discuss recent information concerning the proteome of the presynaptic active zone, focusing on proteins that are potentially involved in the short- and long-term structural modulation of the mature presynaptic compartment. In addition, we discuss the functional relevance of amyloid precursor protein in these membrane fractions and the putative interplay with direct or indirect interaction partners in the active zone.

摘要

突触小泡是化学信号传递中的关键细胞器,使神经元能够相互通信以及与邻近细胞进行通信。小泡的完整或膜相关蛋白介导细胞器在其生命周期中完成的各种任务。这些任务包括细胞器运输、与神经末梢细胞骨架的相互作用、小分子成分的摄取和储存,以及在胞吐和胞吞过程中与突触前质膜、活性区的调节相互作用。过去 30 年来,几个实验室的综合工作导致了突触小泡隔室的蛋白质组学的分子和功能特征。如今,膜蛋白分离和质谱技术的进步极大地推动了这一领域的发展,导致了突触小泡蛋白质组的详细描述,并使突触小泡成为特征描述最详细的细胞器。最近,使用对接的突触小泡作为免疫分离的靶标,鉴定了活性区的蛋白质组。通过凝胶基蛋白分离技术、质谱和免疫检测相结合,在活性区中检测到了相当多种类的蛋白质。这些蛋白质包括突触小泡蛋白、突触前融合和回收机制的成分、参与细胞内信号转导的蛋白质、大量的粘附分子以及可能参与调节突触前功能和结构动态的蛋白质。在这里,我们讨论了关于突触前活性区蛋白质组的最新信息,重点讨论了可能涉及成熟突触前隔室的短期和长期结构调节的蛋白质。此外,我们还讨论了淀粉样前体蛋白在这些膜片中的功能相关性,以及其与活性区中直接或间接相互作用伙伴的潜在相互作用。

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