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Effects of intracellular expression of anti-huntingtin antibodies of various specificities on mutant huntingtin aggregation and toxicity

机译:各种特异性抗亨廷顿蛋白细胞内表达对突变亨廷顿蛋白聚集和毒性的影响

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摘要

We have generated eight mAbs (MW1-8) that bind the epitopes polyglutamine (polyQ), polyproline (polyP), or the C terminus of exon 1 in huntingtin (htt) protein. In the brains of Huntington's disease (HD) mouse models, the anti-polyQ mABs bind to various cytoplasmic compartments, whereas the anti-polyP and anti-C terminus mAbs bind nuclear inclusions containing htt. To use these mAbs as intracellular perturbation agents, we have cloned and expressed the antigen-binding domains of three of the mAbs as single-chain variable region fragment Abs (scFvs). In 293 cells cotransfected with htt exon 1 containing an expanded polyQ domain, MW1, MW2, and MW7 scFvs colocalize with htt exon 1. Moreover, these scFvs coimmunoprecipitate with htt exon 1 in cell extracts. In perturbation experiments, MW7 scFv, recognizing the polyP domains of htt, significantly inhibits aggregation as well as the cell death induced by mutant htt protein. In contrast, MW1 and MW2 scFvs, recognizing the polyQ stretch, stimulate htt aggregation and apoptosis. Therefore, these anti-htt scFvs can be used to investigate the role of the polyP and polyQ domains in HD pathogenesis, and antibody binding to the polyP domain has potential therapeutic value in HD.
机译:我们已经产生了8个单克隆抗体(MW1-8),它们与亨廷顿蛋白(htt)蛋白中的表位聚谷氨酰胺(polyQ),聚脯氨酸(polyP)或外显子1的C末端结合。在亨廷顿舞蹈病(HD)小鼠模型的大脑中,抗polyQ mAB与各种细胞质区室结合,而抗polyP和抗C末端mAb与含有htt的核内含物结合。要将这些mAb用作细胞内扰动剂,我们已经克隆并表达了三个mAb的抗原结合结构域作为单链可变区片段Abs(scFvs)。在用含有扩展的polyQ域的htt外显子1共转染的293细胞中,MW1,MW2和MW7 scFv与htt外显子1共定位。此外,这些scFv在细胞提取物中与htt外显子1共免疫沉淀。在微扰实验中,MWT scFv识别了htt的polyP结构域,显着抑制了聚集以及突变的htt蛋白诱导的细胞死亡。相反,MW1和MW2 scFvs识别了polyQ延伸,刺激了htt聚集和凋亡。因此,这些抗htt scFv可用于研究polyP和polyQ结构域在HD发病机理中的作用,并且与polyP结构域结合的抗体在HD中具有潜在的治疗价值。

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