Tan Duan-Jun, Chang Julia, Liu Ling-Ling, Bai Ren-Kui, Wang Yu-Fen, Yeh Kun-Tu, Wong Lee-Jun C
Institute for Molecular and Human Genetics, Georgetown University Medical Center, Washington DC, USA.
BMC Cancer. 2006 Apr 18;6:93. doi: 10.1186/1471-2407-6-93.
The roles of mitochondria in energy metabolism, the generation of ROS, aging, and the initiation of apoptosis have implicated their importance in tumorigenesis. In this study we aim to establish the mutation spectrum and to understand the role of somatic mtDNA mutations in esophageal cancer.
The entire mitochondrial genome was screened for somatic mutations in 20 pairs (18 esophageal squamous cell carcinomas, one adenosquamous carcinoma and one adenocarcinoma) of tumor/surrounding normal tissue of esophageal cancers, using temporal temperature gradient gel electrophoresis (TTGE), followed by direct DNA sequencing to identify the mutations.
Fourteen somatic mtDNA mutations were identified in 55% (11/20) of tumors analyzed, including 2 novel missense mutations and a frameshift mutation in ND4L, ATP6 subunit, and ND4 genes respectively. Nine mutations (64%) were in the D-loop region. Numerous germline variations were found, at least 10 of them were novel and five were missense mutations, some of them occurred in evolutionarily conserved domains. Using real-time quantitative PCR analysis, the mtDNA content was found to increase in some tumors and decrease in others. Analysis of molecular and other clinicopathological findings does not reveal significant correlation between somatic mtDNA mutations and mtDNA content, or between mtDNA content and metastatic status.
Our results demonstrate that somatic mtDNA mutations in esophageal cancers are frequent. Some missense and frameshift mutations may play an important role in the tumorigenesis of esophageal carcinoma. More extensive biochemical and molecular studies will be necessary to determine the pathological significance of these somatic mutations.
线粒体在能量代谢、活性氧生成、衰老及细胞凋亡启动过程中的作用表明其在肿瘤发生中具有重要意义。在本研究中,我们旨在确定突变谱并了解体细胞线粒体DNA(mtDNA)突变在食管癌中的作用。
采用时间温度梯度凝胶电泳(TTGE)对20对(18例食管鳞状细胞癌、1例腺鳞癌和1例腺癌)食管癌肿瘤/周围正常组织进行体细胞突变筛查,随后进行直接DNA测序以鉴定突变。
在55%(11/20)分析的肿瘤中鉴定出14个体细胞mtDNA突变,分别包括ND4L、ATP6亚基和ND4基因中的2个新的错义突变和1个移码突变。9个突变(64%)位于D环区域。发现了许多种系变异,其中至少10个是新的,5个是错义突变,其中一些发生在进化保守结构域。通过实时定量PCR分析,发现一些肿瘤中的mtDNA含量增加,而另一些肿瘤中的mtDNA含量减少。对分子及其他临床病理结果的分析未显示体细胞mtDNA突变与mtDNA含量之间,或mtDNA含量与转移状态之间存在显著相关性。
我们的结果表明食管癌中体细胞mtDNA突变很常见。一些错义突变和移码突变可能在食管癌的肿瘤发生中起重要作用。需要进行更广泛的生化和分子研究以确定这些体细胞突变的病理意义。
