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巴松管蛋白,一种新型锌指CAG/谷氨酰胺重复蛋白,选择性定位于突触前神经末梢的活性区。

Bassoon, a novel zinc-finger CAG/glutamine-repeat protein selectively localized at the active zone of presynaptic nerve terminals.

作者信息

tom Dieck S, Sanmartí-Vila L, Langnaese K, Richter K, Kindler S, Soyke A, Wex H, Smalla K H, Kämpf U, Fränzer J T, Stumm M, Garner C C, Gundelfinger E D

机构信息

Leibniz Institute for Neurobiology, D-39118 Magdeburg, Germany.

出版信息

J Cell Biol. 1998 Jul 27;142(2):499-509. doi: 10.1083/jcb.142.2.499.

Abstract

The molecular architecture of the cytomatrix of presynaptic nerve terminals is poorly understood. Here we show that Bassoon, a novel protein of >400,000 Mr, is a new component of the presynaptic cytoskeleton. The murine bassoon gene maps to chromosome 9F. A comparison with the corresponding rat cDNA identified 10 exons within its protein-coding region. The Bassoon protein is predicted to contain two double-zinc fingers, several coiled-coil domains, and a stretch of polyglutamines (24 and 11 residues in rat and mouse, respectively). In some human proteins, e.g., Huntingtin, abnormal amplification of such poly-glutamine regions causes late-onset neurodegeneration. Bassoon is highly enriched in synaptic protein preparations. In cultured hippocampal neurons, Bassoon colocalizes with the synaptic vesicle protein synaptophysin and Piccolo, a presynaptic cytomatrix component. At the ultrastructural level, Bassoon is detected in axon terminals of hippocampal neurons where it is highly concentrated in the vicinity of the active zone. Immunogold labeling of synaptosomes revealed that Bassoon is associated with material interspersed between clear synaptic vesicles, and biochemical studies suggest a tight association with cytoskeletal structures. These data indicate that Bassoon is a strong candidate to be involved in cytomatrix organization at the site of neurotransmitter release.

摘要

突触前神经末梢细胞基质的分子结构目前还知之甚少。在此我们表明,巴松管蛋白(一种分子量大于400,000的新型蛋白质)是突触前细胞骨架的一个新组分。小鼠巴松管蛋白基因定位于9F染色体。与相应的大鼠cDNA比较,在其蛋白质编码区内鉴定出10个外显子。预测巴松管蛋白含有两个双锌指结构、几个卷曲螺旋结构域以及一段多聚谷氨酰胺序列(大鼠和小鼠中分别为24个和11个残基)。在一些人类蛋白质中,例如亨廷顿蛋白,此类多聚谷氨酰胺区域的异常扩增会导致迟发性神经退行性变。巴松管蛋白在突触蛋白制剂中高度富集。在培养的海马神经元中,巴松管蛋白与突触小泡蛋白突触素以及突触前细胞基质组分 piccolo 共定位。在超微结构水平上,在海马神经元的轴突终末检测到巴松管蛋白,它在活性区附近高度集中。突触体的免疫金标记显示,巴松管蛋白与散布在清亮突触小泡之间的物质相关联,生化研究表明它与细胞骨架结构紧密结合。这些数据表明,巴松管蛋白很可能参与神经递质释放部位的细胞基质组织形成。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/73ed/2133055/09b184018f01/JCB9804046.f1.jpg

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