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Comparative genomic hybridization-based oncogenetic tree model for genetic classification of breast cancer.

机译:基于比较基因组杂交的癌基因树模型对乳腺癌进行遗传分类。

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OBJECTIVE: To describe a genetic progression pathway in breast cancer by a maximum likelihood-based tree model representing the dependencies between chromosomal imbalances. STUDY DESIGN: One hundred six cases were studied by comparative genomic hybridization, followed by maximum likelihood estimation of an oncogenetic tree model. RESULTS: The tree model identified 3 clusters with correlated chromosomal imbalances. The first cluster included losses at 4q, 5q, 6q, 9p, 13q and a gain at 17q; the second cluster included gains at 1q, 8q, 16p and 20q; the third cluster included losses at 8p, 11q, 16q and 18q. The imbalances nearest the root of the tree were the loss at 13q (cluster 1), the gain at 1q (cluster 2) and the loss at 18q (cluster 3), reflecting an early change in breast cancer evolution. Cox regression analysis revealed the tumor stage and the grade as relevant for overall survival (p = 0.001) and the tumor stage, the grade and the loss at 16q as relevant for disease-free survival (p = 0.001). CONCLUSION: Methods like oncogenetic tree analysis provide insights into the genetic progression of breast cancer and may extract relevant markers detected by screening methods like comparative genomic hybridization for further studies.
机译:目的:通过基于最大似然的树模型来描述乳腺癌的遗传进展途径,该模型代表了染色体失衡之间的依赖性。研究设计:通过比较基因组杂交研究了166例病例,然后对致癌树模型进行了最大似然估计。结果:该树模型确定了3个具有相关染色体失衡的簇。第一组包括4q,5q,6q,9p,13q的损失和17q的收益;第二类包括1q,8q,16p和20q的增益;第三类包括8p,11q,16q和18q的损失。最接近树根的失衡是在13q处丢失(群集1),在1q处丢失(群集2)和在18q处丢失(群集3),这反映了乳腺癌进化的早期变化。 Cox回归分析显示,肿瘤分期和等级与总生存期相关(p = 0.001),肿瘤分期,等级和16q处的损失与无病生存期相关(p = 0.001)。结论:癌基因树分析等方法可洞悉乳腺癌的遗传进展,并可提取通过比较基因组杂交等筛选方法检测到的相关标志物,以供进一步研究。

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