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Flicker-assisted localization microscopy reveals altered mitochondrial architecture in hypertension

机译:闪烁辅助定位显微镜显示高血压患者线粒体结构改变

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摘要

Mitochondrial morphology is central to normal physiology and disease development. However, in many live cells and tissues, complex mitochondrial structures exist and morphology has been difficult to quantify. We have measured the shape of electrically-discrete mitochondria, imaging them individually to restore detail hidden in clusters and demarcate functional boundaries. Stochastic “flickers” of mitochondrial membrane potential were visualized with a rapidly-partitioning fluorophore and the pixel-by-pixel covariance of spatio-temporal fluorescence changes analyzed. This Flicker-assisted Localization Microscopy (FaLM) requires only an epifluorescence microscope and sensitive camera. In vascular myocytes, the apparent variation in mitochondrial size was partly explained by densely-packed small mitochondria. In normotensive animals, mitochondria were small spheres or rods. In hypertension, mitochondria were larger, occupied more of the cell volume and were more densely clustered. FaLM provides a convenient tool for increased discrimination of mitochondrial architecture and has revealed mitochondrial alterations that may contribute to hypertension.
机译:线粒体形态对正常生理和疾病发展至关重要。然而,在许多活细胞和组织中,存在复杂的线粒体结构,并且形态学难以量化。我们测量了电离散线粒体的形状,分别对其进行成像,以恢复隐藏在簇中的细节并划分功能边界。线粒体膜电位的随机“闪烁”通过快速分配的荧光团可视化,并分析了时空荧光变化的逐像素协方差。这种闪烁辅助定位显微镜(FaLM)仅需要落射荧光显微镜和灵敏的照相机。在血管心肌细胞中,线粒体大小的明显变化部分由密集的小线粒体解释。在血压正常的动物中,线粒体是小球或棒。在高血压中,线粒体较大,占据更多的细胞体积,并且聚集更密集。 FaLM提供了一种方便的工具,用于增加对线粒体结构的区分,并揭示了可能导致高血压的线粒体改变。

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