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首页> 外文期刊>Journal of Cancer Research and Clinical Oncology >Mitochondrial DNA analysis efficiently contributes to the identification of metastatic contralateral breast cancers
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Mitochondrial DNA analysis efficiently contributes to the identification of metastatic contralateral breast cancers

机译:线粒体DNA分析有效地有助于鉴定转移性对侧乳腺癌

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Purpose In daily practice, a contralateral breast cancer (CBC) is usually considered as a new independent tumor despite the indications of several studies showing that the second neoplasia may be a metastatic spread of the primary tumor. Recognition of clonal masses in the context of multiple synchronous or metachronous tumors is crucial for correct prognosis, therapeutic choice, and patient management. Mitochondrial DNA (mtDNA) sequencing shows high informative potential in the diagnosis of synchronous neoplasms, based on the fact that somatic mtDNA mutations are non-recurrent events, whereas tumors sharing them have a common origin. We here applied this technique to reveal clonality of the CBC with respect to the first tumor. Methods We analyzed 30 sample pairs of primary breast cancers and synchronous or metachronous CBCs with detailed clinical information available and compared standard clinico-pathological criteria with mtDNA sequencing to reveal the metastatic nature of CBCs. Results MtDNA analysis was informative in 23% of the cases, for which it confirmed a clonal origin of the second tumor. In addition, it allowed to solve two ambiguous cases where histopathological criteria had failed to be conclusive and to suggest a clonal origin for two additional cases that had been classified as independent by pathologists. Conclusion Overall, the mtDNA-based classification showed a more accurate predictive power than standard histopathology in identifying cases of metastatic rather than bilateral breast cancers in our cohort, suggesting that mtDNA sequencing may be a more precise and easy-to-use method to be introduced in daily routine to support and improve histopathological diagnoses.
机译:目的在日常实践中,对侧乳腺癌(CBC)通常被认为是一种新的独立肿瘤,尽管多项研究表明,第二次肿瘤形成可能是原发肿瘤的转移扩散。在多发同步或异时性肿瘤中识别克隆性肿块对于正确的预后、治疗选择和患者管理至关重要。线粒体DNA(mtDNA)测序在同步性肿瘤的诊断中显示出很高的信息潜力,因为体细胞线粒体DNA突变是非复发性事件,而共享它们的肿瘤有一个共同的起源。我们在这里应用这项技术来揭示CBC相对于第一个肿瘤的克隆性。方法我们分析了30对原发性乳腺癌和同步或异时性乳腺癌的临床资料,并将标准临床病理标准与mtDNA测序进行比较,以揭示乳腺癌的转移性质。结果23%的病例进行了MtDNA分析,证实了第二个肿瘤的克隆起源。此外,它还解决了两个组织病理学标准不能确定的模棱两可的病例,并为另外两个被病理学家归类为独立的病例提出了克隆起源的建议。结论总体而言,在我们的队列中,基于mtDNA的分类在识别转移性乳腺癌而非双侧乳腺癌病例方面显示出比标准组织病理学更准确的预测能力,这表明mtDNA测序可能是一种更精确、更易用的方法,可以在日常工作中引入,以支持和改善组织病理学诊断。

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