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一种分泌型补体控制相关蛋白可确保乙酰胆碱受体聚集。

A secreted complement-control-related protein ensures acetylcholine receptor clustering.

作者信息

Gendrel Marie, Rapti Georgia, Richmond Janet E, Bessereau Jean-Louis

机构信息

ENS, Biology Department, Paris, F-75005 France.

出版信息

Nature. 2009 Oct 15;461(7266):992-6. doi: 10.1038/nature08430. Epub 2009 Sep 30.

DOI:10.1038/nature08430
PMID:19794415
Abstract

Efficient neurotransmission at chemical synapses relies on spatial congruence between the presynaptic active zone, where synaptic vesicles fuse, and the postsynaptic differentiation, where neurotransmitter receptors concentrate. Diverse molecular systems have evolved to localize receptors at synapses, but in most cases, they rely on scaffolding proteins localized below the plasma membrane. A few systems have been suggested to control the synaptic localization of neurotransmitter receptors through extracellular interactions, such as the pentraxins that bind AMPA receptors and trigger their aggregation. However, it is not yet clear whether these systems have a central role in the organization of postsynaptic domains in vivo or rather provide modulatory functions. Here we describe an extracellular scaffold that is necessary to cluster acetylcholine receptors at neuromuscular junctions in the nematode Caenorhabditis elegans. It involves the ectodomain of the previously identified transmembrane protein LEV-10 (ref. 6) and a novel extracellular protein, LEV-9. LEV-9 is secreted by the muscle cells and localizes at cholinergic neuromuscular junctions. Acetylcholine receptors, LEV-9 and LEV-10 are interdependent for proper synaptic localization and physically interact based on biochemical evidence. Notably, the function of LEV-9 relies on eight complement control protein (CCP) domains. These domains, also called 'sushi domains', are usually found in proteins regulating complement activity in the vertebrate immune system. Because the complement system does not exist in protostomes, our results suggest that some of the numerous uncharacterized CCP proteins expressed in the mammalian brain might be directly involved in the organization of the synapse, independently from immune functions.

摘要

化学突触处高效的神经传递依赖于突触前活性区(突触小泡在此融合)与突触后分化区(神经递质受体在此聚集)之间的空间一致性。多种分子系统已经进化出来,用于将受体定位在突触处,但在大多数情况下,它们依赖于定位在质膜下方的支架蛋白。有人提出一些系统通过细胞外相互作用来控制神经递质受体的突触定位,比如结合AMPA受体并触发其聚集的五聚体蛋白。然而,这些系统在体内突触后结构域的组织中是否起核心作用,还是仅仅提供调节功能,目前尚不清楚。在这里,我们描述了一种细胞外支架,它是线虫秀丽隐杆线虫神经肌肉接头处乙酰胆碱受体聚集所必需的。它涉及先前鉴定的跨膜蛋白LEV-10(参考文献6)的胞外结构域和一种新的细胞外蛋白LEV-9。LEV-9由肌肉细胞分泌,并定位在胆碱能神经肌肉接头处。根据生化证据,乙酰胆碱受体、LEV-9和LEV-10在突触定位上相互依赖且存在物理相互作用。值得注意的是,LEV-9的功能依赖于八个补体控制蛋白(CCP)结构域。这些结构域,也称为“寿司结构域”,通常存在于调节脊椎动物免疫系统补体活性的蛋白质中。由于原口动物不存在补体系统,我们的结果表明,哺乳动物大脑中表达的众多未表征的CCP蛋白中的一些可能直接参与突触的组织,而与免疫功能无关。

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