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Ultra rapid in vivo screening for anti-Alzheimer anti-amyloid drugs

机译:体内筛选抗阿尔茨海默抗淀粉样蛋白药物的超快速

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摘要

More than 46 million people worldwide suffer from Alzheimer's disease. A large number of potential treatments have been proposed; among these, the inhibition of the aggregation of amyloid β-peptide (Aβ), considered one of the main culprits in Alzheimer's disease. Limitations in monitoring the aggregation of Aβ in cells and tissues restrict the screening of anti-amyloid drugs to in vitro studies in most cases. We have developed a simple but powerful method to track Aβ aggregation in vivo in real-time, using bacteria as in vivo amyloid reservoir. We use the specific amyloid dye Thioflavin-S (Th-S) to stain bacterial inclusion bodies (IBs), in this case mainly formed of Aβ in amyloid conformation. Th-S binding to amyloids leads to an increment of fluorescence that can be monitored. The quantification of the Th-S fluorescence along the time allows tracking Aβ aggregation and the effect of potential anti-aggregating agents.
机译:超过4600万人全世界患有阿尔茨海默病。已经提出了大量潜在的治疗方法;其中,抑制淀粉样蛋白β-肽(Aβ)的聚集,认为Alzheimer疾病中的主要罪魁祸首之一。在大多数情况下,监测细胞和组织中Aβ聚集的限制限制了抗淀粉样蛋白药物在大多数情况下进行体外研究。我们开发了一种简单但有力的方法,可以实时地在体内追踪Aβ聚集,使用细菌在体内淀粉样液中的细菌。我们使用特定的淀粉样蛋白染料硫蛋白-S(TH-S)染色细菌包涵体(IBS),在这种情况下主要由Aβ在淀粉样件上形成。与淀粉样蛋白的结合导致可以监测的荧光的增量。沿当时的TH-S荧光的定量允许跟踪Aβ聚集和潜在的抗聚集剂的影响。

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