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[线粒体DNA D环区域突变与肝细胞癌组织中的活性氧水平]

[Mutations in the D-loop region of mitochondrial DNA and the ROS level in the tissue of hepatocellular carcinoma].

作者信息

Huang Xue-Wen, Zhao Qi, Chen Dao-Zhen, Zhang Li-Shan

机构信息

Clinical Laboratory, Huadong Sanatorium of Shanghai, Wuxi, Jiangsu Province 214002, China.

出版信息

Yi Chuan. 2005 Jan;27(1):14-20.

Abstract

To explore the relationship between ROS level and mutations in D-Loop region of mtDNA, mutations in the D-Loop region of mtDNA and the ROS level in primary hepatocarcinoma tissues were studied. We amplified the D-Loop region of mtDNA of 20 hepatocarcinomas and their adjacent tissue by PCR and then sequencing. ROS in tissue was measured by flow cytometry. mtDNA mutations were detected in 40% (8 of 20) tumor samples. 53 point mutations were detected in eight tumour samples, including 2 insertions, 11 deletions and 40 point mutations. 75% point mutations were T-C and C-T transition. They were four microsatellites among the mutations. Mutations in the adjacent tissues were always companied with mutations in tumour tissues. The mutation frequency in tumour tissues was higher than that in adjacent tissue. There was a larger unidentified deletion. The ROS level in hepatocarcinoma tissue was much higher than control (P<0.01). Meanwhile, we found the ROS level in hepatocarcinoma tissues with mutated mtDNA D-Loop was higher than that hepatocarcinoma tissue normal mtDNA D-Loop, and the ROS level in hepatocarcinoma adjacent tissue with mutated mtDNA D-Loop was higher than that in hepatocarcinoma adjacent tissue with normal mtDNA D-Loop. It was concluded that the D-Loop region of mitochondrial DNA was a highly polymorphoric and mutable region and mutation rate was relatively high in patients with hepaticellular carcinoma, and the abnormal ROS level might be the point mutation in the mitochondrial DNA and hepatocarcinogenesis related to ROS.

摘要

为探讨活性氧(ROS)水平与线粒体DNA(mtDNA)D-环区突变之间的关系,研究了原发性肝癌组织中mtDNA D-环区的突变情况及ROS水平。我们通过聚合酶链反应(PCR)扩增了20例肝癌组织及其癌旁组织的mtDNA D-环区,随后进行测序。采用流式细胞术检测组织中的ROS。在40%(20例中的8例)肿瘤样本中检测到mtDNA突变。在8个肿瘤样本中检测到53个点突变,包括2个插入、11个缺失和40个点突变。75%的点突变是T-C和C-T转换。这些突变中有4个微卫星。癌旁组织中的突变总是与肿瘤组织中的突变相伴。肿瘤组织中的突变频率高于癌旁组织。存在一个较大的未识别缺失。肝癌组织中的ROS水平显著高于对照(P<0.01)。同时,我们发现mtDNA D-环区发生突变的肝癌组织中的ROS水平高于mtDNA D-环区正常的肝癌组织,且mtDNA D-环区发生突变的肝癌旁组织中的ROS水平高于mtDNA D-环区正常的肝癌旁组织。得出结论:线粒体DNA的D-环区是一个高度多态且易变的区域,在肝细胞癌患者中突变率相对较高,ROS水平异常可能与线粒体DNA点突变及肝癌发生有关。

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