Human liver mitochondrial RNA synthesized in isolated organelles

International Hepatology Communications Pub Date : 1996-06-01 DOI:10.1016/0928-4346(96)00289-7

Acisclo Pérez-Martos , Antonio L. Andreu , Manuel J. López-Pérez , Josep E. Murio , Simón Schwartz , Julio Montoya

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Abstract

The study of alterations of mitochondrial DNA transcription could be of fundamental interest to understand the molecular mechanisms underlying the impairment of mitochondrial function in liver diseases related to hepatocyte energy production. We show that isolated normal human liver mitochondria, when incubated in the presence of [α-³²P]UTP in an appropriate incubation medium, in which the energy requirements are provided by exogenous ADP in the presence of oxidizable substrates, are able to support RNA synthesis in a way faithfully resembling the in vivo process. The autoradiographic pattern in agarosemethylmercury hydroxide gels of the newly synthesized RNA shows the presence of all the previously described RNAs coded in the mitochondrial genome (ribosomal, messenger and transfer RNAs). We conclude that this system could be of great value to investigate the role of the mitochondrial genome on human liver pathology related to mitochondrial damage.

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在分离细胞器中合成的人肝脏线粒体RNA

线粒体DNA转录改变的研究对于理解与肝细胞能量产生相关的肝脏疾病中线粒体功能损伤的分子机制具有重要意义。我们发现，当分离的正常人类肝脏线粒体在存在[α-32P]UTP的适当培养液中孵育时，其能量需求由存在可氧化底物的外源性ADP提供，能够以一种与体内过程相似的方式支持RNA合成。新合成的RNA在琼脂糖甲基氢氧化汞凝胶中的放射自显影模式显示了线粒体基因组编码的所有先前描述的RNA(核糖体，信使RNA和转移RNA)的存在。我们认为该系统对于研究线粒体基因组在与线粒体损伤相关的人类肝脏病理中的作用具有重要价值。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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International Hepatology Communications

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