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聚集蛋白调节rapsyn与表面乙酰胆碱受体的相互作用,这是细胞骨架锚定和聚集的基础。

Agrin regulates rapsyn interaction with surface acetylcholine receptors, and this underlies cytoskeletal anchoring and clustering.

作者信息

Moransard Martijn, Borges Lucia S, Willmann Raffaella, Marangi P Angelo, Brenner Hans Rudolf, Ferns Michael J, Fuhrer Christian

机构信息

Department of Neurochemistry, Brain Research Institute, University of Zürich, CH-8057 Zürich, Switzerland.

出版信息

J Biol Chem. 2003 Feb 28;278(9):7350-9. doi: 10.1074/jbc.M210865200. Epub 2002 Dec 16.

Abstract

The acetylcholine receptor (AChR)-associated protein rapsyn is essential for neuromuscular synapse formation and clustering of AChRs, but its mode of action remains unclear. We have investigated whether agrin, a key nerve-derived synaptogenic factor, influences rapsyn-AChR interactions and how this affects clustering and cytoskeletal linkage of AChRs. By precipitating AChRs and probing for associated rapsyn, we found that in denervated diaphragm rapsyn associates with synaptic as well as with extrasynaptic AChRs showing that rapsyn interacts with unclustered AChRs in vivo. Interestingly, synaptic AChRs are associated with more rapsyn suggesting that clustering of AChRs may require increased interaction with rapsyn. In similar experiments in cultured myotubes, rapsyn interacted with intracellular AChRs and with unclustered AChRs at the cell surface, although surface interactions are much more prominent. Remarkably, agrin induces recruitment of additional rapsyn to surface AChRs and clustering of AChRs independently of the secretory pathway. This agrin-induced increase in rapsyn-AChR interaction strongly correlates with clustering, because staurosporine and herbimycin blocked both the increase and clustering. Conversely, laminin and calcium induced both increased rapsyn-AChR interaction and AChR clustering. Finally, time course experiments revealed that the agrin-induced increase occurs with AChRs that become cytoskeletally linked, and that this precedes receptor clustering. Thus, we propose that neural agrin controls postsynaptic aggregation of the AChR by enhancing rapsyn interaction with surface AChRs and inducing cytoskeletal anchoring and that this is an important precursor step for AChR clustering.

摘要

乙酰胆碱受体(AChR)相关蛋白rapsyn对于神经肌肉突触的形成以及AChR的聚集至关重要,但其作用方式仍不清楚。我们研究了神经来源的关键突触生成因子聚集蛋白是否影响rapsyn-AChR相互作用,以及这如何影响AChR的聚集和细胞骨架连接。通过沉淀AChR并探测相关的rapsyn,我们发现在去神经支配的膈肌中,rapsyn与突触以及突触外AChR相关联,这表明rapsyn在体内与未聚集的AChR相互作用。有趣的是,突触AChR与更多的rapsyn相关联,这表明AChR的聚集可能需要与rapsyn增加相互作用。在培养的肌管中进行的类似实验中,rapsyn与细胞内AChR以及细胞表面未聚集的AChR相互作用,尽管表面相互作用更为显著。值得注意的是,聚集蛋白可诱导额外的rapsyn募集到表面AChR并使AChR聚集,且与分泌途径无关。聚集蛋白诱导的rapsyn-AChR相互作用增加与聚集密切相关,因为星形孢菌素和除莠霉素可同时阻断这种增加和聚集。相反,层粘连蛋白和钙可同时诱导rapsyn-AChR相互作用增加和AChR聚集。最后,时间进程实验表明,聚集蛋白诱导的增加发生在与细胞骨架连接的AChR上,且这先于受体聚集。因此,我们提出神经聚集蛋白通过增强rapsyn与表面AChR的相互作用并诱导细胞骨架锚定来控制AChR的突触后聚集,且这是AChR聚集的重要前期步骤。

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