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A bispecific immunotweezer prevents soluble PrP oligomers and abolishes prion toxicity

机译:双特异性免疫镊子可防止可溶性PrP低聚物并消除病毒毒性

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摘要

Antibodies to the prion protein, PrP, represent a promising therapeutic approach against prion diseases but the neurotoxicity of certain anti-PrP antibodies has caused concern. Here we describe scPOM-bi, a bispecific antibody designed to function as a molecular prion tweezer. scPOM-bi combines the complementarity-determining regions of the neurotoxic antibody POM1 and the neuroprotective POM2, which bind the globular domain (GD) and flexible tail (FT) respectively. We found that scPOM-bi confers protection to prion-infected organotypic cerebellar slices even when prion pathology is already conspicuous. Moreover, scPOM-bi prevents the formation of soluble oligomers that correlate with neurotoxic PrP species. Simultaneous targeting of both GD and FT was more effective than concomitant treatment with the individual molecules or targeting the tail alone, possibly by preventing the GD from entering a toxic-prone state. We conclude that simultaneous binding of the GD and flexible tail of PrP results in strong protection from prion neurotoxicity and may represent a promising strategy for anti-prion immunotherapy.
机译:病毒蛋白PrP的抗体代表了一种针对病毒疾病的有前途的治疗方法,但是某些抗PrP抗体的神经毒性引起了人们的关注。在这里,我们描述了scPOM-bi,这是一种双特异性抗体,旨在用作分子病毒镊子。 scPOM-bi结合了神经毒性抗体POM1和神经保护性POM2的互补决定区,它们分别结合球状结构域(GD)和柔性尾部(FT)。我们发现,即使病毒病理已经很明显,scPOM-bi仍可为感染病毒的器官型小脑切片提供保护。而且,scPOM-bi阻止了与神经毒性PrP物种相关的可溶性寡聚物的形成。同时靶向GD和FT比同时进行单个分子治疗或单独靶向尾部更有效,这可能是通过防止GD进入易发毒状态。我们得出的结论是,GD与PrP的柔性尾部同时结合会导致对病毒神经毒性的强力保护,并且可能代表了抗-病毒免疫疗法的有前途的策略。

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