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线粒体的结构与功能:其组织与紊乱

Structure and function of mitochondria: their organization and disorders.

作者信息

Ozawa T, Tanaka M, Suzuki H, Nishikimi M

出版信息

Brain Dev. 1987;9(2):76-81. doi: 10.1016/s0387-7604(87)80021-9.

Abstract

In this lecture, recent advances in studies on the structure and function of mitochondria were reviewed. In particular, in order to understand the etiology of mitochondrial myopathies, the mechanism of the biogenesis of the mitochondrial structure with proteins synthesized in mitochondria and in the cytoplasm was discussed; namely, how proteins encoded by mitochondrial DNA are biosynthesized, and how nuclealy encoded proteins are targeted into the appropriate compartments inside the mitochondria. Recent advances in mitochondriology have made it possible to isolate and purify the enzyme complexes and their subunits, which are involved in mitochondrial oxidative phosphorylation. Immunochemical analyses using a specific antibody against each complex or subunit enabled us to detect defects in individual subunits in mitochondria isolated from a small amount of biopsied material. Several examples of molecular defects revealed by these methods in patients with mitochondrial myopathies were presented, and the principles of their therapy are discussed on the basis of the pattern of the defect. Specific antibodies are also a powerful tool for the cloning of the human cDNAs for the subunits in the mitochondrial energy-transducing machinery. This approach will hopefully facilitate elucidation of the genetic defects underlying these disorders.

摘要

在本次讲座中,回顾了线粒体结构与功能研究的最新进展。特别是,为了理解线粒体肌病的病因,探讨了线粒体结构通过线粒体和细胞质中合成的蛋白质进行生物发生的机制;也就是说,线粒体DNA编码的蛋白质是如何生物合成的,以及细胞核编码的蛋白质是如何靶向进入线粒体内适当的区室的。线粒体学的最新进展使得分离和纯化参与线粒体氧化磷酸化的酶复合物及其亚基成为可能。使用针对每种复合物或亚基的特异性抗体进行免疫化学分析,使我们能够在从少量活检材料中分离出的线粒体中检测单个亚基的缺陷。展示了通过这些方法在患有线粒体肌病的患者中发现的几个分子缺陷实例,并根据缺陷模式讨论了其治疗原则。特异性抗体也是克隆线粒体能量转导机制中亚基的人类cDNA的有力工具。这种方法有望促进对这些疾病潜在遗传缺陷的阐明。

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