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首页> 外文期刊>Blood: The Journal of the American Society of Hematology >TP53 alterations in acute myeloid leukemia with complex karyotype correlate with specific copy number alterations, monosomal karyotype, and dismal outcome
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TP53 alterations in acute myeloid leukemia with complex karyotype correlate with specific copy number alterations, monosomal karyotype, and dismal outcome

机译:具有复杂核型的急性髓细胞性白血病中的TP53改变与特异性拷贝数改变,单核型核型和不良转归相关

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摘要

To assess the frequency of TP53 alterations and their correlation with other genetic changes and outcome in acute myeloid leukemia with complex karyotype (CK-AML), we performed integrative analysis using TP53 mutational screening and array-based genomic profiling in 234 CK-AMLs. TP53 mutations were found in 141 of 234 (60%) and TP53 losses were identified in 94 of 234 (40%) CK-AMLs; in total, 164 of 234 (70%) cases had TP53 alterations. TP53-altered CK-AML were characterized by a higher degree of genomic complexity (aberrations per case, 14.30 vs 6.16; P < .0001) and by a higher frequency of specific copy number alterations, such as -5/5q-, -7/7q-, -16/ 16q-, -18/18q-, +1/+1p, and +11/+11q/ amp11q13~25; among CK-AMLs, TP53- altered more frequently exhibited a monosomal karyotype (MK). Patients with TP53 alterations were older and had significantly lower complete remission rates, inferior event-free, relapse-free, and overall survival. In multivariable analysis for overall survival, TP53 alterations, white blood cell counts, and age were the only significant factors. In conclusion, TP53 is the most frequently known altered gene in CK-AML. TP53 alterations are associated with older age, genomic complexity, specific DNAcopy number alterations, MK, and dismal outcome. In multivariable analysis, TP53 alteration is the most important prognostic factor in CK-AML, outweighing all other variables, including the MK category.
机译:为了评估患有复杂核型(CK-AML)的急性髓样白血病的TP53改变的频率及其与其他遗传变化和结果的相关性,我们在234个CK-AML中使用TP53突变筛查和基于阵列的基因组分析进行了综合分析。在234个中的141个(60%)中发现TP53突变,在234个中的94个(40%)CK-AML中发现TP53丢失;在234例病例中,共有164例(70%)发生了TP53改变。 TP53改变的CK-AML的特征是基因组复杂度更高(每例畸变,14.30 vs 6.16; P <.0001)和特定拷贝数变化的频率更高,如-5 / 5q-,-7 / 7q-,-16 / 16q-,-18 / 18q-,+ 1 / + 1p和+ 11 / + 11q / amp11q13〜25;在CK-AML中,TP53-改变更频繁地表现出核型核型(MK)。 TP53改变的患者年龄较大,完全缓解率明显降低,无事件,无复发和总体生存率较低。在总生存期的多变量分析中,TP53改变,白细胞计数和年龄是唯一重要的因素。总之,TP53是CK-AML中最常见的变异基因。 TP53的改变与年龄,基因组复杂性,特定的DNA拷贝数改变,MK和令人沮丧的结果有关。在多变量分析中,TP53改变是CK-AML中最重要的预后因素,其价值超过所有其他变量,包括MK类别。

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