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Formation of morphologically similar globular aggregates from diverse aggregation-prone proteins in mammalian cells

机译:在哺乳动物细胞中由多种易于聚集的蛋白质形成形态相似的球状聚集体

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摘要

Huntington's disease is a progressive neurodegenerative disorder caused by a polyglutamine repeat expansion in the first exon of the huntingtin (Htt) protein. N-terminal Htt peptides with polyglutamine tracts in the pathological range (51–122 glutamines) form high-molecular-weight protein aggregates with fibrillar morphology in vitro, and they form discrete inclusion bodies in a cell-culture model. However, in some studies, formation of discrete Htt inclusions does not correlate well with cell death. We coexpressed N-terminal Htt fragments containing 91 glutamines fused to different affinity tags in HEK293 cells, and we isolated small aggregates by double sequential-affinity chromatography to assure the isolation of multimeric molecules. Transmission electron microscopy and atomic force microscopy revealed the isolated aggregates as globules or clusters of globules 4–50 nm in diameter without any detectable fibrillar species. Because small nonfibrillar oligomers, not mature fibrils, recently have been suggested to be the principal cytotoxic species in neurodegenerative disease, these Htt globular aggregates formed in cells may represent the pathogenic form of mutant Htt.
机译:亨廷顿舞蹈病是由亨廷顿蛋白(Htt)的第一个外显子中的聚谷氨酰胺重复扩增引起的进行性神经退行性疾病。具有在病理范围内的聚谷氨酰胺束的N末端Htt肽(51-122个谷氨酰胺)在体外形成具有原纤维形态的高分子量蛋白聚集体,并在细胞培养模型中形成离散的包涵体。但是,在一些研究中,离散的Htt夹杂物的形成与细胞死亡没有很好的相关性。我们在HEK293细胞中共表达了含91个谷氨酰胺的N-末端Htt片段,这些谷氨酰胺融合了不同的亲和标签,并通过双重连续亲和色谱法分离了小的聚集体,以确保多聚体分子的分离。透射电子显微镜和原子力显微镜显示分离的聚集体为直径为4–50 nm的小球或小球簇,没有任何可检出的原纤维种类。由于最近有人提出小的非原纤维寡聚体而不是成熟的原纤维是神经退行性疾病的主要细胞毒性物质,因此细胞中形成的这些Htt球状聚集体可能代表突变型Htt的致病形式。

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