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A new mtDNA mutation showing accumulation with time and restriction to skeletal muscle.

机译:一个新的mtDNA突变显示随着时间的积累和骨骼肌的限制。

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摘要

We have identified a new mutation in mtDNA, involving tRNALeu(CUN) in a patient manifesting an isolated skeletal myopathy. This heteroplasmic A-->G transition at position 12320 affects the T psi C loop at a conserved site and was not found in 120 controls. Analysis of cultured fibroblasts, white blood cells/platelets, and skeletal muscle showed that only skeletal muscle contained the mutation and that only this tissue demonstrated a biochemical defect of respiratory-chain activity. In a series of four muscle-biopsy specimens taken over a 12-year period, there was a gradual increase, from 70% to 90%, in the overall level of mutation, as well as a marked clinical deterioration. Single-fiber PCR confirmed that the proportion of mutant mtDNA was highest in cytochrome c oxidase-negative fibers. This study, which reports a mutation involving tRNALeu(CUN), demonstrates clearly that mtDNA point mutations can accumulate over time and may be restricted in their tissue distribution. Furthermore, clinical deterioration seemed to follow the increase in the level of mutation, although, interestingly, the appearance of fibers deficient in respiratory-chain activity showed a lag period.
机译:我们已经在一名患者中发现了一个新的mtDNA突变,其中涉及tRNALeu(CUN),该突变表明存在孤立的骨骼肌病。在位置12320处的这种异质A→G过渡影响了保守位点的T psi C环,在120个对照中均未发现。对培养的成纤维细胞,白细胞/血小板和骨骼肌的分析表明,只有骨骼肌含有该突变,并且只有该组织显示出呼吸链活性的生化缺陷。在过去的12年中,在一系列的四个肌肉活检标本中,突变的总体水平从70%逐渐增加到90%,并且临床表现显着恶化。单纤维PCR证实突变体mtDNA的比例在细胞色素c氧化酶阴性纤维中最高。这项研究报告了一个涉及tRNALeu(CUN)的突变,该研究清楚地表明mtDNA点突变可以随时间积累,并且可能在其组织分布中受到限制。此外,尽管突变水平增加,但临床恶化似乎伴随着突变的发生,尽管有趣的是,缺乏呼吸链活性的纤维的出现显示出滞后期。

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