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与NARP相关的8993位点线粒体DNA突变会减缓分离的淋巴母细胞线粒体中ATP的合成速率。

The mitochondrial DNA mutation at 8993 associated with NARP slows the rate of ATP synthesis in isolated lymphoblast mitochondria.

作者信息

Tatuch Y, Robinson B H

机构信息

Department of Biochemistry and Paediatrics, University of Toronto, Ontario, Canada.

出版信息

Biochem Biophys Res Commun. 1993 Apr 15;192(1):124-8. doi: 10.1006/bbrc.1993.1390.

Abstract

Mitochondria were prepared from three lymphoblast cell lines from patients with high percentage copy numbers of the human mtDNA 8993 mutation and compared to those prepared from related and non-related control cell lines. Rates of ATP synthesis with pyruvate/malate, succinate/rotenone, ascorbate/N'N'N'N' tetramethyl phenylene diamine were reduced to 67%, 58% and 54% of the control rates, respectively. The backward reaction measured as oligomycin sensitive ATPase was reduced to an average of 42% of that in controls. This mutation which changes a conserved leucine to an arginine in the putative membrane proton channel of mitochondrial ATPase effectively reduces the overall rate of oxidative phosphorylation.

摘要

从三名人类线粒体DNA 8993突变拷贝数百分比高的患者的淋巴母细胞系中制备线粒体,并与从相关和不相关对照细胞系中制备的线粒体进行比较。丙酮酸/苹果酸、琥珀酸/鱼藤酮、抗坏血酸/N'N'N'N' -四甲基对苯二胺的ATP合成速率分别降至对照速率的67%、58%和54%。以寡霉素敏感ATP酶测定的逆向反应平均降至对照的42%。这种突变在线粒体ATP酶的假定膜质子通道中将一个保守的亮氨酸变为精氨酸,有效地降低了氧化磷酸化的总体速率。

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