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Candidate anti-Aβ fluorene compounds selected from analogs of amyloid imaging agents

机译:候选抗Aβ芴化合物选自淀粉样蛋白显像剂类似物

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摘要

Alzheimer’s disease (AD) is characterized by depositions of β-amyloid (Aβ) aggregates as amyloid in the brain. To facilitate diagnosis of AD by radioligand imaging, several highly specific small-molecule amyloid ligands have been developed. Because amyloid ligands display excellent pharmacokinetics properties and brain bioavailability, and because we have previously shown that some amyloid ligands bind the highly neurotoxic Aβ oligomers (AβO) with high affinities, they may also be valuable candidates for anti-Aβ therapies. Here we identified two fluorene compounds from libraries of amyloid ligands, initially based on their ability to block cell death secondary to intracellular AβO. We found that the lead fluorenes were able to reduce the amyloid burden including the levels of AβO in cultured neurons and in 5xFAD mice. To explain these in vitro and in vivo effects, we found that the lead fluorenes bind and destabilize AβO as shown by electron paramagnetic resonance spectroscopy studies, and block the harmful AβO-synapse interaction. These fluorenes and future derivatives, therefore, have a potential use in AD therapy and research.
机译:阿尔茨海默氏病(AD)的特征是β-淀粉样蛋白(Aβ)聚集体以淀粉样蛋白形式在大脑中沉积。为了促进通过放射性配体成像诊断AD,已经开发了几种高度特异性的小分子淀粉样蛋白配体。由于淀粉样蛋白配体显示出出色的药代动力学特性和大脑生物利用度,并且由于我们先前已经证明一些淀粉样蛋白配体以高亲和力结合高度神经毒性的Aβ低聚物(AβO),因此它们也可能是抗Aβ治疗的有价值的候选药物。在这里,我们从淀粉样蛋白配体库中鉴定出两种芴化合物,最初是基于它们阻止继发于细胞内AβO的细胞死亡的能力。我们发现铅芴能够减少淀粉样蛋白负担,包括培养的神经元和5xFAD小鼠中的AβO水平。为了解释这些体外和体内效应,我们发现铅芴结合并破坏了AβO的稳定性,如电子顺磁共振波谱研究所示,并阻止了有害的AβO-突触相互作用。因此,这些芴及其未来衍生物在AD治疗和研究中具有潜在用途。

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