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首页> 外文期刊>Cellular Oncology: Analytical Cellular Pathology >DNA Amplifications and Aneuploidy, High Proliferative Activity and Impaired Cell Cycle Control Characterize Breast Carcinomas with Poor Prognosis
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DNA Amplifications and Aneuploidy, High Proliferative Activity and Impaired Cell Cycle Control Characterize Breast Carcinomas with Poor Prognosis

机译:DNA扩增和非整倍性,高增殖活性和细胞周期控制受损的特点预后不良的乳腺癌。

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In order to explore whether specific cytogenetic abnormalities can be used to stratify tumors with a distinctly different clinical course, we performed comparative genomic hybridization (CGH) of tumors from patients who were diagnosed with metastatic disease after an interval of less than 2 years or who remained free from distant metastases for more than 10 years. All patients presented with distant metastases after mastectomy indicating that none of the patients in this study was cured and free of remaining tumor cells. Tumors in the group of short‐term survivors showed a higher average number of chromosomal copy alterations compared to the long‐term survivors. Of note, the number of sub‐chromosomal high‐level copy number increases (amplifications) was significantly increased in the group of short‐term survivors. In both short‐ and long‐term survivors recurrent chromosomal gains were mapped to chromosomes 1q, 4q, 8q, and 5p. Copy number changes that were more frequent in the group of short‐term survivors included gains of chromosome 3q, 9p, 11p and 11q and loss of 17p. Our results indicate that low‐ and high grade malignant breast adenocarcinomas are characterized by a specific pattern of chromosomal copy number changes. Furthermore, immunohistochemical evaluation of the expression levels of Ki‐67, p27KIP1, p21WAF1, p53, cyclin A and cyclin E revealed a correlation between increased proliferative activity and poor outcome.
机译:为了探索特定的细胞遗传学异常是否可用于以明显不同的临床过程对肿瘤进行分层,我们对来自诊断为转移性疾病的患者(间隔时间少于2年)或保留的患者进行了比较基因组杂交(CGH)无远处转移超过10年。所有患者在乳房切除术后均出现远处转移,这表明本研究中没有患者可以治愈并且没有残留的肿瘤细胞。与长期存活者相比,短期存活者组中的肿瘤显示出更高的平均染色体拷贝改变数。值得注意的是,短期幸存者组中亚染色体高水平拷贝数增加(扩增)的次数显着增加。在短期和长期幸存者中,复发的染色体增益都映射到染色体1q,4q,8q和5p。在短期幸存者组中更频繁的拷贝数变化包括染色体3q,9p,11p和11q的获得和17p的丧失。我们的结果表明,低度和高度恶性乳腺腺癌的特征在于染色体拷贝数变化的特定模式。此外,对Ki-67,p27KIP1,p21WAF1,p53,cyclin A和cyclin E表达水平的免疫组织化学评估显示,增殖活性与不良预后之间存在相关性。

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