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Rapid detection of Abeta deposits in APP transgenic mice by Hoechst 33342.

机译:Hoechst 33342快速检测APP转基因小鼠中的Abeta沉积物。

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摘要

The accumulation of beta-amyloid (Abeta) is the earliest event seen in the neocortex and hippocampus of Alzheimer's disease (AD) patients. Transgenic mouse models of Abeta deposition are excellent tools for validating pharmacological therapies for reducing Abeta burden. Sensitive and rapid probes should be needed for detecting Abeta plaques ex vivo and in vivo in the transgenic mouse models. However, a thioflavin derivative, Pittsburgh Compound-B (PIB), which is a successful PET tracer for detecting Abeta plaques in AD brains, does not visualize Abeta plaques in APP and PS1/APP transgenic mice. Here, we report that Hoechst 33342, a cell-permeable fluorescent probe for staining DNA and nuclei, also detects Abeta plaques in APP Tg mouse. These findings could allow us to rapidly detect Abeta plaques in AD mouse models, and to develop improved compounds for detecting Abeta plaques in vivo in mouse models.
机译:β-淀粉样蛋白(Abeta)的积累是阿尔茨海默氏病(AD)患者新皮层和海马中最早出现的事件。 Abeta沉积的转基因小鼠模型是验证减少Abeta负担的药理疗法的绝佳工具。在转基因小鼠模型中离体和体内检测Abeta斑块需要灵敏且快速的探针。但是,硫黄素衍生物匹兹堡化合物B(PIB)是一种成功的PET示踪剂,可用于检测AD大脑中的Abeta斑块,但无法在APP和PS1 / APP转基因小鼠中观察到Abeta斑块。在这里,我们报道Hoechst 33342,一种可渗透细胞的荧光探针,用于染色DNA和细胞核,也可在APP Tg小鼠中检测到Abeta斑块。这些发现可以使我们能够快速检测AD小鼠模型中的Abeta斑块,并开发出改进的化合物用于在小鼠模型中体内检测Abeta斑块。

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