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在缺乏rapsyn的小鼠神经肌肉接头处,突触后特化发育失败。

Failure of postsynaptic specialization to develop at neuromuscular junctions of rapsyn-deficient mice.

作者信息

Gautam M, Noakes P G, Mudd J, Nichol M, Chu G C, Sanes J R, Merlie J P

机构信息

Department of Molecular Biology, Washington University Medical School, St. Louis, Missouri 63110, USA.

出版信息

Nature. 1995 Sep 21;377(6546):232-6. doi: 10.1038/377232a0.

Abstract

Of numerous synaptic components that have been identified, perhaps the best-studied are the nicotinic acetylcholine receptors (AChRs) of the vertebrate neuromuscular junction. AChRs are diffusely distributed on embryonic myotubes, but become highly concentrated (approximately 10,000 microns-2) in the postsynaptic membrane as development proceeds. At least two distinct processes contribute to this accumulation. One is local synthesis: subsynaptic muscle nuclei transcribe AChR subunit genes at higher rates than extra-synaptic nuclei, so AChR messenger RNA is concentrated near synaptic sites. Second, once AChRs have been inserted in the membrane, they form high-density clusters by tethering to a subsynaptic cytoskeletal complex. A key component of this complex is rapsyn, a peripheral membrane protein of relative molecular mass 43K (refs 4, 5), which is precisely colocalized with AChRs at synaptic sites from the earliest stages of neuromuscular synaptogenesis. In heterologous systems, expression of recombinant rapsyn leads to clustering of diffusely distributed AChRs, suggesting that rapsyn may control formation of clusters. To assess the role of rapsyn in vivo, we generated and characterized mutant mice with a targeted disruption of the Rapsyn gene. We report that rapsyn is essential for the formation of AChR clusters, but that synapse-specific transcription of AChR subunit genes can proceed in its absence.

摘要

在已确定的众多突触成分中,研究最为深入的或许是脊椎动物神经肌肉接头处的烟碱型乙酰胆碱受体(AChRs)。AChRs在胚胎肌管上呈弥散分布,但随着发育进程,会在突触后膜高度集中(约10,000个/平方微米)。至少有两个不同的过程促成了这种聚集。一个是局部合成:突触下肌核转录AChR亚基基因的速率高于突触外核,因此AChR信使核糖核酸集中在突触部位附近。其次,一旦AChRs插入膜中,它们会通过与突触下细胞骨架复合物相连而形成高密度簇。该复合物的一个关键成分是rapsyn,一种相对分子质量为43K的外周膜蛋白(参考文献4、5),从神经肌肉突触形成的最早阶段起,它就与AChRs在突触部位精确共定位。在异源系统中,重组rapsyn的表达会导致弥散分布的AChRs聚集,这表明rapsyn可能控制簇的形成。为了评估rapsyn在体内的作用,我们生成并鉴定了Rapsyn基因靶向缺失的突变小鼠。我们报告rapsyn对AChR簇的形成至关重要,但在其缺失的情况下,AChR亚基基因的突触特异性转录仍可进行。

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