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Detection of somatic mutations in the mitochondrial DNA control region D-loop in brain tumors: The first report in Malaysian patients

机译:在脑肿瘤中检测线粒体DNA控制区D环中的体细胞突变:马来西亚患者的首次报道

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摘要

Although the role of nuclear-encoded gene alterations has been well documented in brain tumor development, the involvement of the mitochondrial genome in brain tumorigenesis has not yet been fully elucidated and remains controversial. The present study aimed to identify mutations in the mitochondrial DNA (mtDNA) control region D-loop in patients with brain tumors in Malaysia. A mutation analysis was performed in which DNA was extracted from paired tumor tissue and blood samples obtained from 49 patients with brain tumors. The D-loop region DNA was amplified using the PCR technique, and genetic data from DNA sequencing analyses were compared with the published revised Cambridge sequence to identify somatic mutations. Among the 49 brain tumor tissue samples evaluated, 25 cases (51%) had somatic mutations of the mtDNA D-loop, with a total of 48 mutations. Novel mutations that had not previously been identified in the D-loop region (176 A-deletion, 476 C>A, 566 C>A and 16405 A-deletion) were also classified. No significant associations between the D-loop mutation status and the clinicopathological parameters were observed. To the best of our knowledge, the current study presents the first evidence of alterations in the mtDNA D-loop regions in the brain tumors of Malaysian patients. These results may provide an overview and data regarding the incidence of mitochondrial genome alterations in Malaysian patients with brain tumors. In addition to nuclear genome aberrations, these specific mitochondrial genome alterations may also be considered as potential cancer biomarkers for the diagnosis and staging of brain cancers.
机译:尽管核编码基因改变在脑肿瘤发展中的作用已得到充分证明,但线粒体基因组在脑肿瘤发生中的作用尚未得到充分阐明,并且仍存在争议。本研究旨在确定马来西亚脑肿瘤患者的线粒体DNA(mtDNA)控制区D环中的突变。进行了突变分析,其中从配对的肿瘤组织中提取DNA,并从49名脑肿瘤患者的血液样本中提取DNA。使用PCR技术扩增D环区DNA,并将来自DNA测序分析的遗传数据与已发布的修订版Cambridge序列进行比较,以鉴定体细胞突变。在评估的49个脑肿瘤组织样本中,有25例(51%)的mtDNA D环发生了体细胞突变,共有48个突变。还对以前在D环区域未发现的新突变进行了分类(176 A缺失,476 C> A,566 C> A和16405 A缺失)。没有观察到D环突变状态与临床病理参数之间的显着关联。据我们所知,本研究提供了马来西亚患者脑肿瘤中mtDNA D环区域改变的第一个证据。这些结果可能提供有关马来西亚脑瘤患者线粒体基因组改变发生率的概述和数据。除核基因组畸变外,这些特定的线粒体基因组改变也可被视为诊断和分期脑癌的潜在癌症生物标志物。

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