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Functionally different α-synuclein inclusions yield insight into Parkinson’s disease pathology

机译:功能上不同的α-突触核蛋白内含物有助于深入了解帕金森氏病的病理

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摘要

The formation of α-synuclein (α-S) amyloid aggregates, called Lewy bodies (LBs), is a hallmark of Parkinson’s disease (PD). The function of LBs in the disease process is however still unclear; they have been associated with both neuroprotection and toxicity. To obtain insight into this contradiction, we induced the formation of α-S inclusions, using three different induction methods in SH-SY5Y cells and rat-derived primary neuronal cells. Using confocal and STED microscopy we observed induction-dependent differences in α-S inclusion morphology, location and function. The aggregation of α-S in functionally different compartments correlates with the toxicity of the induction method measured in viability assays. The most cytotoxic treatment largely correlates with the formation of proteasome-associated, juxta-nuclear inclusions. With less toxic methods cytosolic deposits that are not associated with the proteasome are more prevalent. The distribution of α-S over at least two different types of inclusions is not limited to cell models, but is also observed in primary neuronal cells and in human mesencephalon. The existence of functionally different LBs, in vivo and in vitro, gives important insights in the impact of Lewy Body formation on neuronal functioning and may thereby provide a platform for discovering therapeutics.
机译:称为路易小体(LB)的α-突触核蛋白(α-S)淀粉样蛋白聚集体的形成是帕金森氏病(PD)的标志。 LB在疾病过程中的功能仍然不清楚。它们与神经保护和毒性有关。为了深入了解这一矛盾,我们使用三种不同的诱导方法在SH-SY5Y细胞和大鼠来源的原代神经元细胞中诱导了α-S内含物的形成。使用共聚焦和STED显微镜,我们观察到诱导依赖性的α-S夹杂物形态,位置和功能的差异。在功能上不同的区室中,α-S的聚集与在活力测定中测量的诱导方法的毒性相关。细胞毒性最大的治疗与蛋白酶体相关,近端核包裹体的形成有关。用毒性较小的方法,与蛋白酶体不相关的胞质沉积物更为普遍。 α-S在至少两种不同类型的夹杂物上的分布不仅限于细胞模型,还可以在原代神经元细胞和人中脑中观察到。体内和体外功能不同的LB的存在,对路易体形成对神经​​元功能的影响提供了重要的见识,从而可能为发现治疗方法提供平台。

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