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分化型甲状腺癌中线粒体DNA突变与年龄因素的关系。

Mitochondrial DNA mutations in differentiated thyroid cancer with respect to the age factor.

作者信息

Witte Jürgen, Lehmann Steffen, Wulfert Michael, Yang Quin, Röher Hans D

机构信息

Department of General and Trauma surgery, Heinrich Heine University, Moorenstrasse 5, 40225 Düsseldorf, Germany.

出版信息

World J Surg. 2007 Jan;31(1):51-9. doi: 10.1007/s00268-005-0447-5.

Abstract

INTRODUCTION

Increased numbers of mitochondria in differentiated thyroid cancer and, most strikingly, mutations in human mitochondrial DNA (mtDNA) in older people have led to speculation that mtDNA mutations might contribute to aging or accumulate in postmitotic tissues with age. Mutation analyses of mtDNA in papillary (PTCs) and follicular (FTCs) thyroid carcinomas have been limited to date. The significance and frequency of mtDNA mutations in PTC and FTC are therefore controversial, as is age dependence.

METHODS

We analyzed eight sample pairs of PTC and six of FTC tissue with the corresponding normal thyroid tissue. DNA was extracted from frozen and formaldehyde-fixed tissue using the QIAmp Tissue Kit. Sequence differences in the mtDNA between tumor and normal tissue were detected using appropriate polymerase chain reaction (PCR) products for heteroduplex analysis in a denaturing high performance liquid chromatography (HPLC) Wave System (Transgenomic). Mutations were confirmed and identified by sequencing the PCR products of conspicuous chromatograms. The samples were obtained from 346 patients with PTC and 105 patients with FTC. We analyzed the whole mitochondrial genome from seven PTC and three FTC tumors along with the corresponding normal thyroid tissue. 3/7 PTC samples showed two heteroplasmic mutations and one polymorphism; all 3 FTCs showed homoplasmic and/or heteroplasmic mutations.

RESULTS

All but one of these tumors are well documented in the mitochondrial database MITOMAP. MtDNA mutations were found in all three patients aged 45 years and older. There was no correlation, however, in this small group to clinical prognostic factors for recurrence and especially for survival in differentiated thyroid carcinomas, such as histology, tumor size, lymph node metastases, distant metastases, and gender, most likely because of the short follow-up. While univariate analysis of the findings in the whole cohort of 346 patients with PTC suggested that age is a significant prognostic factor for survival (P = 0.0237) but not for recurrence (P = 0.65), this was not the case in the 105 patients with FTC.

CONCLUSIONS

Although we found accumulation of mutations in two older patients with PTC and one patient with FTC (all three patients older than 45 years had mtDNA mutations), the low frequency of these mutations in the small group of 10 analyzed patients did not correlate with statistically validated clinical prognosticators for recurrence or survival, especially not with age. The low power of our data are therefore not able to support or refute the hypothesis that these mtDNA mutations are related to age-dependent tumor progression in the thyroid or that they "may be involved in thyroid tumorigenesis."

摘要

引言

分化型甲状腺癌中线粒体数量增加,而且最显著的是,老年人的人类线粒体DNA(mtDNA)发生突变,这引发了人们的猜测,即mtDNA突变可能导致衰老,或者随着年龄增长在有丝分裂后组织中积累。迄今为止,对乳头状(PTC)和滤泡状(FTC)甲状腺癌中mtDNA的突变分析一直有限。因此,PTC和FTC中mtDNA突变的意义和频率存在争议,年龄依赖性也是如此。

方法

我们分析了8对PTC样本和6对FTC样本及其相应的正常甲状腺组织。使用QIAmp组织试剂盒从冷冻和甲醛固定的组织中提取DNA。使用适当的聚合酶链反应(PCR)产物在变性高效液相色谱(HPLC)Wave系统(Transgenomic)中检测肿瘤组织和正常组织之间mtDNA的序列差异,以进行异源双链分析。通过对明显色谱图的PCR产物进行测序来确认和鉴定突变。样本取自346例PTC患者和105例FTC患者。我们分析了7例PTC肿瘤和3例FTC肿瘤及其相应正常甲状腺组织的整个线粒体基因组。7例PTC样本中有3例显示出两种异质性突变和一种多态性;所有3例FTC均显示出纯质性和/或异质性突变。

结果

除其中一个肿瘤外,所有这些肿瘤在mitochondrial数据库MITOMAP中都有详细记录。在所有3例45岁及以上的患者中均发现了mtDNA突变。然而,在这个小群体中,与分化型甲状腺癌复发尤其是生存的临床预后因素没有相关性,例如组织学、肿瘤大小、淋巴结转移、远处转移和性别,很可能是因为随访时间短。虽然对346例PTC患者的整个队列研究结果进行单因素分析表明,年龄是生存的一个显著预后因素(P = 0.0237),但不是复发的预后因素(P = 0.65),而在105例FTC患者中并非如此。

结论

尽管我们在2例老年PTC患者和1例FTC患者中发现了突变积累(所有3例患者年龄均超过45岁且有mtDNA突变),但在这10例分析患者的小群体中,这些突变的低频率与经统计学验证的复发或生存临床预后指标无关,尤其是与年龄无关。因此,我们数据的低效能无法支持或反驳这些mtDNA突变与甲状腺中年龄依赖性肿瘤进展相关或“可能参与甲状腺肿瘤发生”这一假设。

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