Kopsidas G, Kovalenko S A, Kelso J M, Linnane A W
Centre for Molecular Biology and Medicine, Epworth Hospital, 89 Bridge Road, Richmond, Melbourne, Victoria 3121, Australia.
Mutat Res. 1998 Oct 12;421(1):27-36. doi: 10.1016/s0027-5107(98)00150-x.
Post-mitotic tissues such as skeletal muscle develop a tissue bioenergy mosaic during the process of normal aging that eventually culminates into a bioenergetically diverse tissue containing cells ranging in their oxidative phosphorylation capacity from normal to grossly defective. The mosaic is postulated to develop continuously from birth with the relative proportions of cytochrome c oxidase (COX) proficient (positive) and COX deficient (negative) muscle fibers differing dramatically as a function of age. Generally, young individuals only display the rare fiber deficient in COX activity while aged individuals show a significantly higher proportion of negative fibers. There appears to be a random element governing which cells will be affected. Consequently, adjacent cells within a given tissue may exhibit vastly differing COX activities. Multiple mitochondrial DNA (mtDNA) deletions also appear to accumulate in skeletal muscle, similarly displaying a dramatic disparity as a function of age. Our previous findings have indicated that the accumulation of multiple mtDNA deletions, along with a concurrent decrease in wild-type mtDNA, strongly correlates with the age-associated decrease in COX activity observed in skeletal muscle. Although no definitive associations were established at the cellular level, an important prediction arose from this study. Cells that accumulate large numbers of mitochondrial mutations and have reduced levels of full-length mtDNA would be expected to be severely affected and show reduced COX activity as a consequence. Cells that accumulate fewer mutations or retain adequate amounts of wild-type mtDNA would be predicted to be less affected or even retain normal oxidative metabolism. In order to establish a link associating COX activity to the status of mtDNA within individual fibers, we developed single cell extra-long PCR (XL-PCR). The procedure was used to assess the relative concentration of full-length mtDNA with respect to any mtDNA deletions detected in individual human skeletal muscle fibers of 'pre-established' COX activity. Single cell XL-PCR analysis of COX positive fibers dissected from a 5-year old and 90-year old individual showed that 80% or more of the fibers contained full length mtDNA and few, if any, mtDNA rearrangements. COX deficient or COX intermediate fibers taken from the same individuals, by contrast, depicted a heterogeneous population of rearranged mtDNA species with no detectable full-length mtDNA. The data presented here indicates that COX deficient muscle fibers extracted from individuals, regardless of age, were accompanied by extensive mtDNA rearrangements and reduced levels of full-length mtDNA. This provides compelling evidence linking mtDNA mutations to COX activity decline in skeletal muscle and has important implications when considering the molecular basis of the aging process.
有丝分裂后的组织,如骨骼肌,在正常衰老过程中会形成一种组织生物能量镶嵌现象,最终发展成为一种生物能量多样化的组织,其中包含氧化磷酸化能力从正常到严重缺陷不等的细胞。据推测,这种镶嵌现象从出生起就持续发展,细胞色素c氧化酶(COX)功能正常(阳性)和COX功能缺陷(阴性)的肌纤维的相对比例会随着年龄的增长而发生显著变化。一般来说,年轻人仅表现出罕见的COX活性缺陷纤维,而老年人中阴性纤维的比例则显著更高。似乎存在一个随机因素决定哪些细胞会受到影响。因此,给定组织内的相邻细胞可能表现出极大不同的COX活性。多个线粒体DNA(mtDNA)缺失似乎也会在骨骼肌中积累,同样随着年龄的增长呈现出显著差异。我们之前的研究结果表明,多个mtDNA缺失的积累以及野生型mtDNA的同时减少,与骨骼肌中观察到的与年龄相关的COX活性下降密切相关。尽管在细胞水平上未建立明确的关联,但这项研究产生了一个重要预测。预计积累大量线粒体突变且全长mtDNA水平降低的细胞会受到严重影响,进而表现出COX活性降低。预计积累较少突变或保留足够量野生型mtDNA的细胞受到的影响较小,甚至保留正常的氧化代谢。为了建立COX活性与单个纤维内mtDNA状态之间的联系,我们开发了单细胞超长PCR(XL-PCR)。该方法用于评估在“预先确定”COX活性的个体人类骨骼肌纤维中检测到的任何mtDNA缺失情况下全长mtDNA的相对浓度。对从一名5岁和一名90岁个体中分离出的COX阳性纤维进行单细胞XL-PCR分析表明,80%或更多的纤维含有全长mtDNA,几乎没有mtDNA重排。相比之下,从同一受试者获取的COX缺陷或COX中间纤维呈现出重排mtDNA种类各异的群体,未检测到全长mtDNA。此处呈现的数据表明,从个体中提取的COX缺陷肌纤维,无论年龄大小,都伴随着广泛的mtDNA重排和全长mtDNA水平降低。这为将mtDNA突变与骨骼肌中COX活性下降联系起来提供了有力证据,并且在考虑衰老过程的分子基础时具有重要意义。
