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Assessing mitochondria biogenesis.

机译:评估线粒体的生物发生。

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摘要

Mitochondria have their own DNA (mtDNA) and hence biogenesis of mitochondria requires a coordination of nuclear and mtDNA, both of which encode for mitochondria proteins. Our understanding of the molecular control of mitochondria biogenesis has increased in recent years, providing key signatures of the process. To determine whether or not a tissue or an organ of human or animal origin is undergoing mitochondria biogenesis, multiple parameters should be analyzed. First and foremost is visualization and measurement of mitochondria mass/volume in histological sections using fluorescent mitochondria dyes and light microscopy or transmission electron microscopy to yield quantitative results. To confirm or extend these types of analysis, biochemical markers of mitochondria biogenesis should also be included, including assessment of mtDNA copy number, steady-state levels of biogenesis-related transcription factors (e.g. mitochondria transcription factor A, mitochondrial transcription specificity factors, nuclear respiratory factors 1 and 2, and peroxisome proliferator activated receptor gamma coactivator-1-alpha), mtDNA-encoded transcripts and proteins, and rates of mitochondria translation. These techniques are described in isolation and in the context of transgenic and dietary animal models that have been used as tools to study the regulation of mitochondria biogenesis and its role in disease pathology.
机译:线粒体具有自己的DNA(mtDNA),因此线粒体的生物发生需要核和mtDNA的协调,两者均编码线粒体蛋白。近年来,我们对线粒体生物发生的分子控制的了解有所增加,为该过程提供了重要的标志。为了确定人类或动物来源的组织或器官是否正在进行线粒体生物发生,应分析多个参数。首先,最重要的是使用荧光线粒体染料和光学显微镜或透射电子显微镜对组织切片中的线粒体质量/体积进行可视化和测量,以得出定量结果。为了证实或扩展这些类型的分析,还应包括线粒体生物发生的生化标记,包括评估mtDNA拷贝数,与生物发生相关的转录因子(例如线粒体转录因子A,线粒体转录特异性因子,核呼吸道)的稳态水平因子1和2,以及过氧化物酶体增殖物激活的受体γcoactivator-1-alpha),mtDNA编码的转录本和蛋白质以及线粒体翻译的速率。这些技术是在转基因和饮食动物模型的背景下单独描述的,这些模型已用作研究线粒体生物发生的调控及其在疾病病理中的作用的工具。

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