遗传 ›› 2008, Vol. 30 ›› Issue (12): 1557-1562.doi: 10.3724/SP.J.1005.2008.01557

• 研究报告 • 上一篇    下一篇

tRNA 7472delC可能是耳聋与癫痫相关的线粒体基因新突变

赵建越1; 唐霄雯1; 兰金山2; 吕建新1; 杨丽4; 李智渊3; 朱翌1, 3; 孙冬梅1; 杨爱芬1; 王金丹1; 徐静2; 管敏鑫1, 4

  

  1. 1. 温州医学院浙江省医学遗传学重点实验室, 温州 325035;
    2. 衢州人民医院耳鼻喉科, 衢州 32400;
    3. 温州医学院附属第一医院, 温州 325000;
    4. Division and Program in Human Genetic and Center for Hearing and Deafness Research, Cincinnati Children’s Hospital Medical Center, Cininnati, OH45229, USA

  • 收稿日期:2008-03-04 修回日期:2008-08-30 出版日期:2008-12-10 发布日期:2008-12-10
  • 通讯作者: 管敏鑫

Hearing loss and epilepsy may be associated with the novel mito-chondrial tRNA7472delC mutation in a Chinese family

ZHAO Jian-Yue1; TANG Xiao-Wen1; LAN Jin-Shan2; LV Jian-Xin1; YANG Li4; LI Zhi-Yuan3; ZHU Yi1, 3; SUN Dong-Mei1; YANG Ai-Fen1; WANG Jin-Dan1; XU Jing2; GUAN Min-Xin1, 4

  

  1. 1. Zhejiang Provincial Key Laboratory of Medical Genetics, School of Life Sciences, Wenzhou Medical College, Wenzhou 325035, China;
    2. Department of Otolaryngology, Quzhou People’s Hospital, Quzhou 324000, China;
    3. Department of Otolaryngology, the First Affiliated Hospital, Wenzhou Medical College, Wenzhou 325000, China;
    4. Division of Human Genetics and Center for Hearing and Deafness Research, Cincinnati Children’s Hospital Medical Center, Cincinnati Ohio
    45229, USA
  • Received:2008-03-04 Revised:2008-08-30 Online:2008-12-10 Published:2008-12-10
  • Contact: GUAN Min-Xin

摘要:

线粒体DNA突变与许多人类疾病的发病机制相关。文章报道1例典型的患有耳聋与癫痫症状的具有母系遗传特征的中国家系。该家系共3代人, 其中14名母系成员中有3名耳聋患者, 3名癫痫患者, 而其他成员则无临床症状。线粒体全基因组序列分析表明, tRNASer(UCN)基因7472delC新突变和33个多态位点属于东亚单体型B4b1a2。7472delC突变位于tRNASer(UCN)高度保守的T-arm上。而在该区域的相同位点7472insC突变已在多个无遗传相关的家系中被发现与耳聋和癫痫相关。7472insC突变使tRNA代谢和线粒体功能产生缺陷。这样与7472insC突变相近的7472delC突变可能也会以相似机制引起线粒体功能障碍。同时, 在该家系中未发现GJB2基因及其他线粒体基因突变。因此, tRNASer(UCN) 7472delC可能是耳聋与癫痫相关的线粒体基因新突变。

关键词: 耳聋, 癫痫, 线粒体DNA, 7472delC新突变

Abstract:

Mutations in mitochondrial DNA have been associated with a wide spectrum of clinical abnormalities. We reported here the clinical and genetic evaluations as well as mutational analysis of mitochondrial DNA(mtDNA) in a three-generation Chinese Han family with maternally transmitted hearing loss and epilepsy. Of 14 matrilineal relatives, three suffered from hearing loss, three had epilepsy, and other did not have significant clinical abnormalities. Sequence analysis of mitochondrial genome in this family identified the novel 7472delC in tRNASer(UCN) and 33 variants belonging to Asian haplogroup B4b1a2. The 7472delC locates at the highly conserved residue of T-arm of this tRNA. In fact, the 7472insC at the same position of this tRNA has been associated with hearing loss and epilepsy in several genetically unrelated families. The 7472insC has been shown to lead to a failure in tRNA metabolism and mitochondrial dysfunction. Thus, 7472delC mutation, similar to 7472insC mutation, may result in the mitochondrial dysfunctions responsible for the hearing loss and epilepsy. Furthermore, none of mutation in deafness-associated GJB2 gene was detected in this Chinese family. Therefore, the 7472delC is likely a new mitochondrial mutation with hearing loss and epilepsy.