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Visualization of APP and BACE-1 approximation in neurons: new insights into the amyloidogenic pathway

机译:神经元中APP和BACE-1逼近的可视化:淀粉样生成途径的新见解

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摘要

Cleavage of APP (amyloid precursor protein) by BACE-1 (β-site APP cleaving enzyme-1) is the rate-limiting step in amyloid-beta (Aβ) production and a neuropathologic hallmark of Alzheimer's disease (AD); thus physical approximation of this substrate-enzyme pair is a critical event with broad biological and therapeutic implications. Despite much research, neuronal locales of APP/BACE-1 convergence and APP-cleavage remain unclear. Here we report an optical assay – based on fluorescence complementation – to visualize in-cellulo APP/BACE-1 interactions as a simple on/off signal. Combined with other assays tracking the fate of internalized APP in hippocampal neurons, we found that APP/BACE-1 interact in both biosynthetic and endocytic compartments; particularly along recycling-microdomains such as dendritic spines and presynaptic boutons. In axons, APP and BACE-1 are co-transported, and also interact during transit. Finally, our assay reveals that the AD-protective “Icelandic” mutation greatly attenuates APP/BACE-1 interactions, suggesting a mechanistic basis for protection. Collectively, the data challenge canonical models and provide concrete insights into long-standing controversies in the field.
机译:BACE-1(β位APP裂解酶-1)裂解APP(淀粉样前体蛋白)是淀粉样β(Aβ)产生的限速步骤,是阿尔茨海默氏病(AD)的神经病理学标志。因此,该底物-酶对的物理近似是关键事件,具有广泛的生物学和治疗意义。尽管进行了大量研究,但尚不清楚APP / BACE-1收敛和APP切割的神经元位置。在这里,我们报告了一种基于荧光互补的光学检测方法,可将细胞内A​​PP / BACE-1相互作用可视化为简单的开/关信号。结合跟踪海马神经元内在化APP命运的其他检测方法,我们发现APP / BACE-1在生物合成和内吞区室中都相互作用。尤其是沿循环利用微区,例如树突棘和突触前钮扣。在轴突中,APP和BACE-1共转运,并且在转运过程中也相互作用。最后,我们的测定揭示了AD保护性“冰岛”突变大大减弱了APP / BACE-1的相互作用,为保护提供了机理基础。总体而言,数据对规范模型提出了挑战,并为该领域长期存在的争议提供了具体见解。

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