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[耳蜗缺氧与线粒体DNA缺失:导致老年性聋的可能相关因素]

[Cochlear hypoxia and mtDNA deletion: possible correlated factors to cause presbycusis].

作者信息

Dai P, Jiang S, Gu R

机构信息

Otolaryngology Department of Chinese PLA General Hospital, Beijing 100853, China.

出版信息

Zhonghua Yi Xue Za Zhi. 2000 Dec;80(12):897-900.

PMID:11236628
Abstract

OBJECTIVE

To find the relationship among the most common mitochondrial DNA (mtDNA) 4,977 bp deletion, aging and deterioration of acoustic organ and determine the pathologic factors causing mtDNA 4,977 bp deletion.

METHODS

Sixty-seven temporal bones from a presbycusis group, an age-matched control group and a young control group were evaluated. The nested PCR and tri-nested PCR techniques were used to test the presence of mtDNA 4,977 deletion. Computer imaging processing was used to measure the parameters of blood vessels in the internal acoustic meatus.

RESULTS

Temporal bones from patients aged 50 years or over frequently showed mtDNA 4,977 deletions. In presbycusis patients, 17 of 34 ears showed mtDNA 4,977 deletion, whereas only 4 of 19 ears from the age-matched control group showed mtDNA 4,977 deletions. mtDNA 4,977 deletions were often seen in the spiral ganglion and vestibular ganglion neurons. In the presbycusis group, the lumen of the vasa nervosum of the internal auditory meatus showed a more severe reduction in patients with mtDNA 4,977 deletion than in those without deletion.

CONCLUSION

There is a strong correlation between presbycusis and mtDNA 4,977 deletion. We hypothesize that cochlear hypoxia may cause mtDNA 4,977 deletions and other mtDNA mutants which in turn may cause a reduction of mitochondrial oxidative phosphorylation and decreased auditory nerve function. The symptoms of neural presbycusis, however, may appear only after mtDNA metabolism decreases below a specific threshold.

摘要

目的

探寻最常见的线粒体DNA(mtDNA)4977 bp缺失与衰老及听觉器官退变之间的关系,并确定导致mtDNA 4977 bp缺失的病理因素。

方法

对来自老年性聋组、年龄匹配对照组和青年对照组的67块颞骨进行评估。采用巢式PCR和三重巢式PCR技术检测mtDNA 4977缺失的存在情况。利用计算机图像处理技术测量内耳道血管的参数。

结果

50岁及以上患者的颞骨常显示mtDNA 4977缺失。在老年性聋患者中,34只耳中有17只显示mtDNA 4977缺失,而年龄匹配对照组的19只耳中只有4只显示mtDNA 4977缺失。mtDNA 4977缺失常见于螺旋神经节和前庭神经节神经元。在老年性聋组中,mtDNA 4977缺失患者内听道神经血管的管腔缩小比未缺失患者更为严重。

结论

老年性聋与mtDNA 4977缺失之间存在强相关性。我们推测耳蜗缺氧可能导致mtDNA 4977缺失及其他mtDNA突变,进而可能导致线粒体氧化磷酸化减少和听神经功能下降。然而,神经性老年性聋的症状可能仅在mtDNA代谢降至特定阈值以下时才会出现。

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[Cochlear hypoxia and mtDNA deletion: possible correlated factors to cause presbycusis].[耳蜗缺氧与线粒体DNA缺失:导致老年性聋的可能相关因素]
Zhonghua Yi Xue Za Zhi. 2000 Dec;80(12):897-900.
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Correlation of cochlear blood supply with mitochondrial DNA common deletion in presbyacusis.老年性聋中耳蜗血供与线粒体DNA常见缺失的相关性
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Association of mitochondrial DNA deletions and cochlear pathology: a molecular biologic tool.线粒体DNA缺失与耳蜗病理学的关联:一种分子生物学工具。
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The role of mitochondrial DNA large deletion for the development of presbycusis in Fischer 344 rats.线粒体DNA大片段缺失在Fischer 344大鼠老年性聋发生发展中的作用。
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