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首页> 外文期刊>British Journal of Cancer >Relationship between 3p deletions and telomerase activity in non-small-cell lung cancer: prognostic implications
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Relationship between 3p deletions and telomerase activity in non-small-cell lung cancer: prognostic implications

机译:非小细胞肺癌3p缺失与端粒酶活性之间的关系:预后意义。

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3p deletions and telomerase reactivation are two of the most frequent events described in relation to non-small-cell lung cancer (NSCLC) pathogenesis. Moreover, a number of genes that map on 3p have been proposed as candidates to tumour-suppressor genes of importance in the lung cancer process. In this work, we analysed deletions at different 3p loci in relationship to telomerase activity in 66 NSCLCs obtained from patients who had suffered potentially curative surgery. Also, we evaluated prognostic implications. DNA samples were analysed for 3p deletions using five different polymorphic human dinucleotide repeat DNA markers (D3S1619 at 3p22.2, D3S3623 at 3p22.1, D3S1260 at 3p21.33, D3S3697 at 3p14.3, and D3S3722 at 3p21.2). Telomerase activity was investigated by a TRAP-based method. Possible correlations between the different molecular markers and distributions of disease-free survival were estimated. Our data revealed a significant correlation between telomerase activity and losses of heterozygosity (LOH) on D3S3697 (P=0.040), since all of the tumours showing deletion at this locus were positives for telomerase. Moreover, our results revealed clear associations with poor prognosis of patients, in the case of LOH at D3S1260 and D3S3697 (P=0.005 and 0.005, respectively). According to our data, potential repressors for telomerase may be located in chromosome 3p.
机译:3p缺失和端粒酶再激活是与非小细胞肺癌(NSCLC)发病机理有关的两个最常见事件。而且,已经提出了许多定位在3p上的基因作为在肺癌过程中重要的肿瘤抑制基因的候选者。在这项工作中,我们分析了从患有潜在治愈性手术的患者中获得的66例NSCLC中与端粒酶活性相关的不同3p位点的缺失。此外,我们评估了预后意义。使用五个不同的多态性人二核苷酸重复DNA标记(3p22.2处的D3S1619、3p22.1处的D3S3623、3p21.33处的D3S1260、3p14.3处的D3S3697和3p11.2处的D3S3722)分析了DNA样品的3p缺失。通过基于TRAP的方法研究端粒酶活性。估计了不同分子标记与无病生存期分布之间的可能相关性。我们的数据显示端粒酶活性与D3S3697上的杂合性(LOH)丧失之间存在显着相关性(P = 0.040),因为在该位点显示缺失的所有肿瘤均为端粒酶阳性。此外,我们的结果显示,在D3S1260和D3S3697的LOH情况下,患者的不良预后明显相关(分别为P = 0.005和0.005)。根据我们的数据,端粒酶的潜在阻遏物可能位于3p染色体上。

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