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The potential role for use of mitochondrial DNA copy number as predictive biomarker in presbycusis

机译:线粒体DNA拷贝数在老年性痴呆中作为预测性生物标志物的潜在作用

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Objectives: Age-related hearing impairment, or presbycusis, is the most common communication disorder and neurodegenerative disease in the elderly. Its prevalence is expected to increase, due to the trend of growth of the elderly population. The current diagnostic test for detection of presbycusis is implemented after there has been a change in hearing sensitivity. Identification of a pre-diagnostic biomarker would raise the possibility of preserving hearing sensitivity before damage occurs. Mitochondrial dysfunction, including the production of reactive oxygen species and induction of expression of apoptotic genes, participates in the progression of presbycusis. Mitochondrial DNA sequence variation has a critical role in presbycusis. However, the nature of the relationship between mitochondrial DNA copy number, an important biomarker in many other diseases, and presbycusis is undetermined. Methods: Fifty-four subjects with presbycusis and 29 healthy controls were selected after ear, nose, throat examination and pure-tone audiometry. DNA was extracted from peripheral blood samples. The copy number of mitochondrial DNA relative to the nuclear genome was measured by quantitative real-time polymerase chain reaction. Results: Subjects with presbycusis had a lower median mitochondrial DNA copy number than healthy subjects and the difference was statistically significant ( P =0.007). Mitochondrial DNA copy number was also significantly associated with degree of hearing impairment ( P =0.025) and audiogram configuration ( P =0.022). Conclusion: The findings of this study suggest that lower mitochondrial DNA copy number is responsible for presbycusis through alteration of mitochondrial function. Moreover, the significant association of mitochondrial DNA copy number in peripheral blood samples with the degree of hearing impairment and audiogram configuration has potential for use as a standard test for presbycusis, providing the possibility of the development of an easy-to-use biomarker for the early detection of this condition.
机译:目的:与年龄有关的听力障碍或老年性耳聋是老年人中最常见的沟通障碍和神经退行性疾病。由于老年人口的增长趋势,预计其患病率会增加。听力敏感度发生变化后,将进行当前的诊断为老年性耳聋的诊断测试。预先诊断的生物标志物的鉴定将增加在损伤发生之前保留听力敏感性的可能性。线粒体功能障碍,包括活性氧的产生和凋亡基因表达的诱导,参与了老年性痴呆的发展。线粒体DNA序列变异在老花眼中起关键作用。但是,线粒体DNA拷贝数(许多其他疾病中的重要生物标志物)与老年性痴呆之间关系的性质尚未确定。方法:通过耳,鼻,喉检查和纯音测听,选择54名老年性耳聋患者和29名健康对照者。从外周血样品中提取DNA。通过定量实时聚合酶链反应测量相对于核基因组的线粒体DNA的拷贝数。结果:老花眼受试者的线粒体DNA拷贝数中位数低于健康受试者,且差异具有统计学意义(P = 0.007)。线粒体DNA拷贝数也与听力障碍程度(P = 0.025)和听力图配置(P = 0.022)显着相关。结论:这项研究的结果表明,线粒体DNA拷贝数较低是通过改变线粒体功能导致老年性耳聋的原因。此外,外周血样品中线粒体DNA拷贝数与听力障碍程度和听力图配置的显着相关性有可能用作老年性耳聋的标准检测方法,为开发易于使用的生物标志物提供了可能性。尽早发现这种情况。

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