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High expression of HMGA2 independently predicts poor clinical outcomes in acute myeloid leukemia

机译:HMGA2的高表达独立预测急性髓性白血病的临床预后不良

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In acute myeloid leukemia (AML), risk stratification based on cytogenetics and mutation profiling is essential but remains insufficient to select the optimal therapy. Accurate biomarkers are needed to improve prognostic assessment. We analyzed RNA sequencing and survival data of 430 AML patients and identified HMGA2 as a novel prognostic marker. We validated a quantitative PCR test to study the association of HMGA2 expression with clinical outcomes in 358 AML samples. In this training cohort, HMGA2 was highly expressed in 22.3% of AML, mostly in patients with intermediate or adverse cytogenetics. High expression levels of HMGA2 (H?+?) were associated with a lower frequency of complete remission (58.8% vs 83.4%, P??0.001), worse 3-year overall survival (OS, 13.2% vs 43.5%, P??0.001) and relapse-free survival (RFS, 10.8% vs 44.2%, P??0.001). A positive HMGA2 test also identified a subgroup of patients unresponsive to standard treatments. Multivariable analyses showed that H?+?was independently associated with significantly worse OS and RFS, including in the intermediate cytogenetic risk category. These associations were confirmed in a validation cohort of 260 patient samples from the UK NCRI AML17 trial. The HMGA2 test could be implemented in clinical trials developing novel therapeutic strategies for high-risk AML.
机译:在急性髓细胞性白血病(AML)中,基于细胞遗传学和突变图谱的风险分层至关重要,但仍不足以选择最佳疗法。需要准确的生物标志物以改善预后评估。我们分析了430例AML患者的RNA测序和生存数据,并将HMGA2确定为一种新的预后标志物。我们验证了定量PCR测试的准确性,以研究HMGA2表达与358例AML样品的临床结局之间的关系。在该训练队列中,HMGA2在22.3%的AML中高表达,主要发生在具有中等或不良细胞遗传学的患者中。 HMGA2的高表达水平(H + +)与完全缓解的频率较低(58.8%vs 83.4%,P 0.001),3年总生存期较差(OS,13.2%vs 43.5%,P ≤0.001)和无复发生存率(RFS,10.8%vs 44.2%,P≤0.001)。 HMGA2测试阳性也可识别出对标准治疗无反应的患者亚组。多变量分析表明,H + +与显着恶化的OS和RFS独立相关,包括中等细胞遗传学风险类别。这些关联在来自UK NCRI AML17试验的260个患者样本的验证队列中得到证实。 HMGA2测试可以在开发针对高危AML的新型治疗策略的临床试验中实施。

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