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A Twin Study of Mitochondrial DNA Polymorphisms Shows that Heteroplasmy at Multiple Sites Is Associated with mtDNA Variant 16093 but Not with Zygosity

机译：线粒体DNA多态性的一项双胞胎研究表明，多个位点的异质性与mtDNA变体16093相关，但与合子性无关

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The mitochondrial theory of ageing proposes that damage to mitochondria and diminished mitochondrial DNA (mtDNA) repair are major contributors to cellular dysfunction and age-related diseases. We investigate the prevalence of heteroplasmy in the mtDNA control region in buccal swab and blood derived samples for 178 women from the TwinsUK cohort (41 DZ pair 39 MZ pairs, 18 singletons, mean age 57.5 range 28–82) and its relationship to age, BMI and fasting insulin and glucose serum levels. The overall estimated prevalence of heteroplasmy for both tissues in the control region measured for 37 sites was 17%. The prevalence of heteroplasmy was higher among the older half of the study subjects than in the younger half (23% vs 10% p<0.03), primarily reflecting the increase in the prevalence of a heteroplasmic dinucleotide CA repeat in variable region II (VRII) with age. The VRII 523–524 heteroplasmic site (heteroplasmic in 25 subjects) was also associated with a decrease in BMI. In addition, concordance rates for common heteroplasmy were observed to be near complete for both dizygotic (DZ = 94%) and monozygotic twin pairs (MZ = 100%), consistent with previous reports that suggest variation in heteroplasmy rates between generations are determined by bottlenecks in maternal transmission of mitochondria. Differences in the prevalence of heteroplasmy were observed overall between samples derived from buccal swabs (19%) and blood (15%, p<0.04). These were particularly marked at position 16093 of hypervariable region I (HVI, 7% vs 0%, respectively, p<4×10⁻¹¹). The presence of the C allele at position 16093 in blood was associated with the presence of heteroplasmy in buccal swabs at this position (p = 3.5×10⁻¹⁴) and also at VRII (p = 2×10⁻⁴) suggesting a possible predisposing role for this site in the accumulation of heteroplasmy. Our data indicate that BMI is potentially associated with control region heteroplasmy.

机译：线粒体衰老理论认为，线粒体的损伤和线粒体DNA（mtDNA）修复的减少是造成细胞功能障碍和与年龄有关的疾病的主要因素。我们调查了TwinsUK队列中178名妇女（41 DZ对39 MZ对，18单身，平均年龄57.5范围28-82）在口腔拭子和血液样本中mtDNA控制区域中异质性的普遍性及其与年龄的关系， BMI和空腹胰岛素和葡萄糖血清水平。在37个部位的对照区域中，两种组织的异质性总体估计患病率为17％。在研究对象的上半部分，异质性患病率高于年轻的一半（23％比10％，p <0.03），这主要反映了可变区II（VRII）中异质性二核苷酸CA重复序列的患病率增加。随着年龄的增长。 VRII 523–524异质位点（25名受试者为异质位）也与BMI降低相关。此外，对于双合子（DZ = 94％）和单卵双生子对（MZ = 100％），常见异质性的一致性率都接近完成，这与以前的报道表明世代之间异质性率的变化是由瓶颈决定的一致。在线粒体的母体传播中。从颊拭子（19％）和血液（15％，p <0.04）获得的样品之间总体上观察到异质性患病率的差异。这些在高变区I的位置16093处特别显着（HVI，分别为7％和0％，p <4×10 ^{-11 ）。血液中16093位的C等位基因的存在与该位置颊拭子的异质性存在（p = 3.5×10 ^{−14 ）以及VRII（p = 2×10） ^{−4 ）表明该位点在异质性积累中可能具有诱发作用。我们的数据表明BMI可能与控制区域异质性相关。}}}

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期刊名称 PLoS Clinical Trials
作者
Toby Andrew; Cassandra D. Calloway; Sarah Stuart; Sang Hoon Lee; Raj Gill; Gail Clement; Philip Chowienczyk; Tim D. Spector; Ana M. Valdes;
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年(卷),期 2008(6),8
年度 2008
页码 e22332
总页数 8
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1. Mitochondrial DNA Variation and Heteroplasmy in Monozygotic Twins Clinically Discordant for Multiple Sclerosis [J] . Souren Nicole Y. P., Gerdes Lisa A., Kuempfel Tania, Human mutation . 2016,第8期

机译：单卵双胞胎的线粒体DNA变异和异质性在多发性硬化症临床上不一致。
2. Reduced Stimulation of Recombinant DNA Polymerase γ and Mitochondrial DNA (mtDNA) Helicase by Variants of Mitochondrial Single-stranded DNA-binding Protein (mtSSB) Correlates with Defects in mtDNA Replication in Animal Cells [J] . Marcos T. Oliveira, Laurie S. Kaguni The Journal of biological chemistry . 2011,第47期

机译：通过线粒体单链DNA结合蛋白（MTSSB）的变体与动物细胞中MTDNA复制中的缺陷相关，减少了重组DNA聚合酶γ和线粒体DNA（MTDNA）螺旋酶的刺激
3. Modulating mtDNA heteroplasmy by mitochondria-targeted restriction endonucleases in a 'differential multiple cleavage-site' model. [J] . Bacman SR, Williams SL, Hernandez D, Gene therapy . 2007,第18期

机译：通过线粒体靶向限制性核酸内切酶在“差异多切割位点”模型中调节mtDNA异质性。
4. Characterization of mtDNA SNP typing using quantitative real-time PCR with special emphasis on heteroplasmy detection and mixture ratio assessment [C] . H. Niederstatter, T.J. Parsons, W. Parso International Society for Forensic Genetics . 2006

机译：用定量实时PCR键入MTDNA SNP键入特异性强调异质检测和混合比评估
5. Analysis of polymorphisms and heteroplasmy in mitochondrial DNA for human identification. [D] . Calloway, Cassandra Danelle. 2009

机译：线粒体DNA多态性和异质性分析，以供人类识别。
6. Modulating mtDNA heteroplasmy by mitochondria-targeted restriction endonucleases in a ‘differential multiple cleavage-site’ model [O] . SR Bacman, SL Williams, D Hernandez, -1

机译：在差异多切割位点模型中通过线粒体靶向的限制性核酸内切酶调控mtDNA的异质性
7. A twin study of mitochondrial DNA polymorphisms shows that heteroplasmy at multiple sites is associated with mtDNA variant 16093 but not with zygosity. [O] . Toby Andrew, Cassandra D Calloway, Sarah Stuart, 2011

机译：线粒体DNa多态性的双胞胎研究表明，多个位点的异质性与mtDNa变体16093相关，但与接合性无关。

A Twin Study of Mitochondrial DNA Polymorphisms Shows that Heteroplasmy at Multiple Sites Is Associated with mtDNA Variant 16093 but Not with Zygosity

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