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Large-Scale Oral Treatment Study with the Four Most Promising D3-Derivatives for the Treatment of Alzheimer's Disease

机译:大规模口腔治疗研究与治疗阿尔茨海默病的四个最有前途的D3衍生物

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Alzheimer's disease (AD) is a progressive neurodegenerative disorder that is associated with the aggregation of the amyloid beta protein (A beta). A beta oligomers are currently thought to be the major neurotoxic agent responsible for disease development and progression. Thus, their elimination is highly desirable for therapy development. Our therapeutic approach aims at specific and direct elimination of toxic A beta oligomers by stabilizing A beta monomers in an aggregation-incompetent conformation. We have proven that our lead compound "D3", an all D-enantiomeric-peptide, specifically eliminates A beta oligomers in vitro. In vivo, D3 enhances cognition and reduces plaque load in several transgenic AD mouse models. Here, we performed a large-scale oral proof of concept efficacy study, in which we directly compared four of the most promising D3-derivatives in transgenic mice expressing human amyloid precursor protein with Swedish and London mutations (APP(SL)), transgenic mice, to identify the most effective compound. RD2 and D3D3, both derived from D3 by rational design, were discovered to be the most effective derivatives in improving cognition in the Morris water maze. The performance of RD2- and D3D3-treated mice within the Morris water maze was significantly better than placebo-treated mice and, importantly, nearly as good as those of non-transgenic littermates, suggesting a complete reversal of the cognitive deficit of APPSL mice.
机译:阿尔茨海默病(AD)是一种渐进神经退行性疾病,与淀粉样蛋白β蛋白(β)的聚集有关。目前认为β低聚物是负责疾病发展和进展的主要神经毒剂。因此,他们的消除是治疗发展的非常理想的。我们的治疗方法通过稳定β单体在聚集 - 无化的构象中来确定毒β低聚物的具体和直接消除。我们已经证明,我们的铅化合物“D3”,一种全部D-映体肽,具体地消除体外β低聚物。体内,D3增强了认知并减少了几种转基因AD小鼠模型中的斑块载荷。在这里,我们进行了大规模的概念疗效研究证明,其中我们直接与瑞典和伦敦突变表达人淀粉样蛋白前体蛋白的转基因小鼠中最有前途的D3衍生物(App(SL)),转基因小鼠,识别最有效的化合物。通过理性设计衍生自D3的RD2和D3D3,被发现是改善Morris水迷宫中的认知的最有效衍生物。莫里斯水迷宫内的RD2和D3D3处理的小鼠的表现明显优于安慰剂处理的小鼠,重要的是,几乎与非转基因凋落物一样好,表明APPSL小鼠的认知缺陷完全逆转。

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