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Accumulation of point mutations in mitochondrial DNA of aging mice.

机译:衰老小鼠线粒体DNA中点突变的积累。

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Mitochondrial DNA (mtDNA) exists in a highly genotoxic environment created by exposure to reactive oxygen species, somewhat deficient DNA repair, and the relatively low fidelity of polymerase gamma. Given the severity of the environment, it was anticipated that mutation accumulation in the mtDNA of aging animals should exceed that of nuclear genes by several orders of magnitude. We have analyzed fragments amplified from the D-loop region of mtDNA from 2 to 22-month-old mice. The amplified 432 bp fragments were cloned into plasmid vectors, and plasmid DNAs from individual clones were purified and sequenced. None of 110 fragments from young mice contained a mutation, while 9 of 87 clones originating from old animals contained base substitutions (chi square = 11.9, P<0.001). The estimated mutation frequency in mtDNA from old mice was 11.6+/-2.7 or 25.4+/-7.8 per 10(5) nucleotides (depending on assumptions of clonality), which exceeds existing estimates for mutation frequencies for nuclear genes by approximately 1000-fold. Our data suggest that at 22 months of age, which roughly corresponds to 3/4 of the mouse natural life span, most mtDNA molecules carry multiple point mutations.
机译:线粒体DNA(mtDNA)存在于高度遗传毒性的环境中,这种环境是由于暴露于活性氧,DNA修复略有缺陷以及聚合酶γ的保真度较低而造成的。考虑到环境的严重性,预计衰老动物的mtDNA中的突变积累应比核基因的突变积累高几个数量级。我们分析了从2至22个月大的小鼠的mtDNA D环区域扩增的片段。将扩增的432 bp片段克隆到质粒载体中,并对来自各个克隆的质粒DNA进行纯化和测序。来自年幼小鼠的110个片段中没有一个包含突变,而源自年老动物的87个克隆中有9个具有碱基取代(卡方= 11.9,P <0.001)。老年小鼠的mtDNA的估计突变频率为每10(5)个核苷酸11.6 +/- 2.7或25.4 +/- 7.8(取决于克隆性的假设),比核基因突变频率的现有估计值高约1000倍。我们的数据表明,在22个月大时(大约相当于小鼠自然寿命的3/4),大多数mtDNA分子带有多点突变。

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