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首页> 外文期刊>Mutation Research: International Journal on Mutagenesis, Chromosome Breakage and Related Subjects >Cellular phenotypes of age-associated skeletal muscle mitochondrial abnormalities in rhesus monkeys.
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Cellular phenotypes of age-associated skeletal muscle mitochondrial abnormalities in rhesus monkeys.

机译:恒河猴中与年龄相关的骨骼肌线粒体异常的细胞表型。

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Rhesus monkey vastus lateralis muscle was examined histologically for age-associated electron transport system (ETS) abnormalities: fibers lacking cytochrome c oxidase activity (COX(-)) and/or exhibiting succinate dehydrogenase hyperreactivity (SDH(++)). Two hundred serial cross-sections (spanning 1600 &mgr;m) were obtained and analyzed for ETS abnormalities at regular intervals. The abundance and length of ETS abnormal regions increased with age. Extrapolating the data to the entire length of the fiber, up to 60% of the fibers were estimated to display ETS abnormalities in the oldest animal studied (34 years) compared to 4% in a young adult animal (11 years). ETS abnormal phenotypes varied with age and fiber type. Middle-aged animals primarily exhibited the COX(-) phenotype, while COX(-)/SDH(++) abnormalities were more common in old animals. Transition region phenotype was affected by fiber type with type 2 fibers first displaying COX(-) and then COX(-)/SDH(++) while type 1 fibers progressed from normal to SDH(++) and then to COX(-)/SDH(++). In situ hybridizations studies revealed an association of ETS abnormalities with deletions of the mitochondrial genome. By measuring cross-sectional area along the length of ETS abnormal fibers, we demonstrated that some of these fibers exhibit atrophy. Our data suggest mitochondrial (mtDNA) deletions and associated ETS abnormalities are contributors to age-associated fiber atrophy.
机译:组织学检查了恒河猴股外侧肌的年龄相关的电子传输系统(ETS)异常:纤维缺乏细胞色素c氧化酶活性(COX(-))和/或表现出琥珀酸脱氢酶高反应性(SDH(++))。获得了200个连续横截面(跨度1600μm),并定期进行ETS异常分析。 ETS异常区域的丰度和长度随年龄增长而增加。将数据外推到纤维的整个长度,据估计,研究的最老的动物(34岁)中多达60%的纤维表现出ETS异常,而成年成年动物(11岁)中有4%的纤维表现出ETS异常。 ETS异常表型随年龄和纤维类型而异。中年动物主要表现出COX(-)表型,而COX(-)/ SDH(++)异常在老年动物中更为常见。过渡区表型受纤维类型的影响,其中2型纤维先显示COX(-),然后显示COX(-)/ SDH(++),而1型纤维从正常显示为SDH(++),然后显示为COX(-)。 / SDH(++)。原位杂交研究表明,ETS异常与线粒体基因组缺失有关。通过测量沿ETS异常纤维长度的横截面积,我们证明其中一些纤维表现出萎缩。我们的数据表明线粒体(mtDNA)缺失和相关的ETS异常是与年龄相关的纤维萎缩的原因。

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