首页> 美国卫生研究院文献>The Journal of Biological Chemistry >The Glycine-Alanine Dipeptide Repeat from C9orf72 Hexanucleotide Expansions Forms Toxic Amyloids Possessing Cell-to-Cell Transmission Properties
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The Glycine-Alanine Dipeptide Repeat from C9orf72 Hexanucleotide Expansions Forms Toxic Amyloids Possessing Cell-to-Cell Transmission Properties

机译:从C9orf72六核苷酸扩展的甘氨酸-丙氨酸二肽重复形成具有细胞间传递特性的有毒淀粉样蛋白

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摘要

Hexanucleotide expansions, GGGGCC, in the non-coding regions of the C9orf72 gene were found in major frontotemporal lobar dementia and amyotrophic lateral sclerosis patients (C9FTD/ALS). In addition to possible RNA toxicity, several dipeptide repeats (DPRs) are translated through repeat-associated non-ATG-initiated translation. The DPRs, including poly(GA), poly(GR), poly(GP), poly(PR), and poly(PA), were found in the brains and spinal cords of C9FTD/ALS patients. Among the DPRs, poly(GA) is highly susceptible to form cytoplasmic inclusions, which is a characteristic of C9FTD/ALS. To elucidate DPR aggregation, we used synthetic (GA)15 DPR as a model system to examine the aggregation and structural properties in vitro. We found that (GA)15 with 15 repeats fibrillates rapidly and ultimately forms flat, ribbon-type fibrils evidenced by transmission electron microscopy and atomic force microscopy. The fibrils are capable of amyloid dye binding and contain a characteristic cross-β sheet structure, as revealed by x-ray scattering. Furthermore, using neuroblastoma cells, we demonstrated the neurotoxicity and cell-to-cell transmission property of (GA)15 DPR. Overall, our results show the structural and toxicity properties of GA DPR to facilitate future DPR-related therapeutic development.
机译:在主要额颞叶性痴呆和肌萎缩性侧索硬化症患者(C9FTD / ALS)中发现了C9orf72基因非编码区的六核苷酸扩增GGGGCC。除了可能的RNA毒性外,还通过重复相关的非ATG启动的翻译来翻译几个二肽重复(DPR)。在C9FTD / ALS患者的大脑和脊髓中发现了DPR,包括poly(GA),poly(GR),poly(GP),poly(PR)和poly(PA)。在DPR中,poly(GA)非常容易形成胞质内含物,这是C9FTD / ALS的特征。为了阐明DPR聚集,我们使用合成(GA)15 DPR作为模型系统,以在体外检查聚集和结构特性。我们发现具有15个重复序列的(GA)15快速原纤化并最终形成扁平的带状原纤维,这由透射电子显微镜和原子力显微镜证明。如X射线散射所揭示的,该原纤维能够与淀粉样蛋白染料结合并且含有特征性的交叉β折叠结构。此外,使用成神经细胞瘤细胞,我们证明了(GA)15 DPR的神经毒性和细胞间传递特性。总体而言,我们的结果显示了GA DPR的结构和毒性,可促进未来与DPR相关的治疗发展。

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