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Do DNA copy number changes differentiate uterine from non-uterine leiomyosarcomas and predict metastasis?

机译:DNA拷贝数变化是否将子宫与非子宫平滑肌肉瘤区分开来并预测转移?

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DNA copy number changes were investigated in 51 (19 uterine and 32 nonuterine) primary leiomyosarcomas by comparative genomic hybridization. The aim was to evaluate whether true biological differences exist between uterine and nonuterine leiomyosarcoma and whether changes revealed by comparative genomic hybridization have prognostic value. Genomic imbalances were found in 48 (94%) cases. The most frequent DNA copy number changes were losses in 10q (35%), 13q (57%), and 16q (41%), gains in 1q (41%), and gains and high-level amplifications in 17p (39%). Gains were nearly as frequent as losses in both uterine and nonuterine leiomyosarcoma. Correlation-based tree modeling revealed two clusters that segregated significantly a group of uterine (gains at 1q11–q24) and a group of nonuterine (losses at 13q14–q34, 16q11.1–q24, and 10q21–q26) cases. The nonuterine cluster was associated with subcutaneous origin and a trend toward increased metastasis-free survival. Further explorative analyses identified aberrations associated with shorter metastasis-free survival time, including losses at 2q32.1–q37 and gains at 8q24.1–q24.3, whereas the cases with losses at 6cen-p25 showed longer metastasis-free survival time.
机译:通过比较基因组杂交研究了51例(19例子宫和32例非子宫)平滑肌肉瘤的DNA拷贝数变化。目的是评估子宫和非子宫平滑肌肉瘤之间是否存在真正的生物学差异,以及通过比较基因组杂交揭示的变化是否具有预后价值。发现基因组失衡的案例有48个(94%)。 DNA拷贝数变化最频繁的是10q(35%),13q(57%)和16q(41%)的损失,1q(41%)的增加以及17p(39%)的增加和高水平扩增。子宫平滑肌肉瘤和非子宫平滑肌肉瘤的收益几乎与损失一样频繁。基于相关性的树模型显示,两个簇将一组子宫(在1q11–q24处获得收益)和一组非子宫(在13q14-q34、16q11.1-q24和10q21-q26处丢失)明显分隔开。非子宫簇与皮下起源和无转移生存增加趋势有关。进一步的探索性分析确定了与无转移生存时间较短相关的像差,包括2q32.1–q37损失和8q24.1–q24.3损失,而6cen-p25损失的病例显示无转移生存时间更长。

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