Development of a 213Bi-Labeled Pyridyl Benzofuran for Targeted α-Therapy of Amyloid-β Aggregates.

Aidan A Bender, Emily K Kirkeby, Donna J Cross, Satoshi Minoshima, Andrew G Roberts, Tara E Mastren
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Abstract

Alzheimer disease is a neurodegenerative disorder with limited treatment options. It is characterized by the presence of several biomarkers, including amyloid-β aggregates, which lead to oxidative stress and neuronal decay. Targeted α-therapy (TAT) has been shown to be efficacious against metastatic cancer. TAT takes advantage of tumor-localized α-particle emission to break disease-associated covalent bonds while minimizing radiation dose to healthy tissues due to the short, micrometer-level, distances traveled. We hypothesized that TAT could be used to break covalent bonds within amyloid-β aggregates and facilitate natural plaque clearance mechanisms. Methods: We synthesized a 213Bi-chelate-linked benzofuran pyridyl derivative (BiBPy) and generated [213Bi]BiBPy, with a specific activity of 120.6 GBq/μg, dissociation constant of 11 ± 1.5 nM, and logP of 0.14 ± 0.03. Results: As the first step toward the validation of [213Bi]BiBPy as a TAT agent for the reduction of Alzheimer disease-associated amyloid-β, we showed that brain homogenates from APP/PS1 double-transgenic male mice (6-9 mo old) incubated with [213Bi]BiBPy exhibited a marked reduction in amyloid-β plaque concentration as measured using both enzyme-linked immunosorbent and Western blotting assays, with a half-maximal effective concentration of 3.72 kBq/pg. Conclusion: This [213Bi]BiBPy-concentration-dependent activity shows that TAT can reduce amyloid plaque concentration in vitro and supports the development of targeting systems for in vivo validations.

开发用于淀粉样蛋白-β聚集体靶向α治疗的 213Bi 标记吡啶基苯并呋喃
阿尔茨海默病是一种神经退行性疾病,治疗方法有限。其特征是存在多种生物标志物,包括淀粉样蛋白-β聚集体,从而导致氧化应激和神经元衰亡。靶向α疗法(TAT)已被证明对转移性癌症有效。靶向α治疗利用肿瘤定位的α粒子发射来打破与疾病相关的共价键,同时因其短距离、微米级的传输距离而将健康组织所受的辐射剂量降至最低。我们假设 TAT 可用于打破淀粉样蛋白-β 聚集体中的共价键,并促进天然斑块清除机制。方法:我们合成了一种213Bi-螯合物连接的苯并呋喃吡啶衍生物(BiBPy),并生成了[213Bi]BiBPy,其比活度为120.6 GBq/μg,解离常数为11 ± 1.5 nM,logP为0.14 ± 0.03。结果:作为验证[213Bi]BiBPy 作为减少阿尔茨海默病相关淀粉样蛋白-β的 TAT 剂的第一步,我们发现,[213Bi]BiBPy 在阿尔茨海默病相关淀粉样蛋白-β患者的脑匀浆中的浓度为 0.5%、我们发现,用[213Bi]BiBPy培养的APP/PS1双转基因雄性小鼠(6-9月龄)的脑匀浆显示出淀粉样蛋白-β斑块浓度的明显降低。72 kBq/pg。结论这种[213Bi]BiBPy浓度依赖性活性表明,TAT可以降低体外淀粉样斑块的浓度,并支持开发用于体内验证的靶向系统。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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