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Detection of Amyloid β Oligomers with RNA Aptamers in AppNL-G-F/NL-G-F Mice: A Model of Arctic Alzheimer’s Disease

机译:APPN1-G-F / NL-G-F小鼠中RNA适体的淀粉样蛋白β低聚体的检测:北极患者疾病模型

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RNA aptamers have garnered attention for diagnostic applications due to their ability to recognize diverse targets. Oligomers of 42-mer amyloid β-protein (Aβ42), whose accumulation is relevant to the pathology of Alzheimer’s disease (AD), are among the most difficult molecules for aptamer recognition because they are prone to aggregate in heterogeneous forms. In addition to designing haptens for in vitro selection of aptamers, the difficulties involved in determining their effect on Aβ42 oligomerization impede aptamer research. We previously developed three RNA aptamers (E22P-AbD4, -AbD31, and -AbD43) with high affinity for protofibrils (PFs) derived from a toxic Aβ42 dimer. Notably, these aptamers recognized diffuse staining, which likely originated from PFs or higher-order oligomers with curvilinear structures in a knock-in App~(NL-G-F/NL-G-F) mouse, carrying the Arctic mutation that preferentially induced the formation of PFs, in addition to a PS2Tg2576 mouse. To determine which oligomeric sizes were mainly altered by the aptamer, ion mobility–mass spectrometry (IM–MS) was carried out. One aptamer, E22P-AbD43, formed adducts with the Aβ42 monomer and dimer, leading to suppression of further oligomerization. These findings support the utility of these aptamers as diagnostics for AD.
机译:由于能够识别不同的目标,RNA Aptamers因识别诊断应用而受到关注。 42-MEL淀粉样蛋白β-蛋白(Aβ42)的低聚物,其积累与阿尔茨海默病(AD)的病理相关,是适体识别的最困难的分子中,因为它们易于以异质形式骨料聚集。除了设计哈维斯的体外选择适体的选择外,涉及确定其对Aβ42寡聚化的影响的困难阻碍了适体研究。我们以前开发了具有高亲和力的三个RNA适体(E22P-ABD4,-ABD31和-ABD43),其用于衍生自有毒Aβ42二聚体的原生纤维(PFS)。值得注意的是,这些适体识别弥漫染色,其可能来自PFS或高阶低聚物,其在敲入的APP〜(NL-GF / NL-GF)小鼠中具有曲线结构,携带优先诱导PFS形成的北极突变,除了PS2TG2576鼠标之外。为了确定主要由适体改变哪种低聚尺寸,进行离子迁移率质谱(IM-MS)。一种适体,E22P-ABD43,用Aβ42单体和二聚体形成加合物,导致抑制进一步的寡聚化。这些调查结果支持这些适体的实用程序作为广告的诊断。

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