Minimal Residual Disease Quantitation in Acute Myeloid Leukemia

David Shook , Elaine Coustan-Smith , Raul C. Ribeiro , Jeffrey E. Rubnitz , Dario Campana
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引用次数: 47

Abstract

The prognosis for patients with acute myeloid leukemia (AML) is heterogeneous. A minority of patients have clinical and biologic features associated with a very high risk of relapse. For the remaining patients, no clear prognostic factors can be identified at diagnosis. The degree of treatment response is likely to be an informative predictor of outcome for these patients. Modern assays to detect AML cells that are undetectable by conventional morphologic techniques, ie, minimal residual disease (MRD), can potentially improve measurements of treatment response. It is plausible that modifications to treatment based on the results of these assays will improve clinical management and ultimately increase cure rates. Established MRD assays for AML are based on either polymerase chain reaction amplification of genetic abnormalities or flow cytometric detection of abnormal immunophenotypes. Residual disease and treatment response can be measured by these assays in a manner that is much more sensitive and objective than that afforded by conventional morphologic examination. The expanding use of MRD testing is beginning to change the definitions of treatment response and of remission. Other clinically informative uses of MRD testing include the detection of early relapse and the evaluation of the efficacy of new antileukemic agents.

急性髓系白血病微量残留病定量分析
急性髓性白血病(AML)患者的预后是不均匀的。少数患者具有与复发风险非常高相关的临床和生物学特征。对于其余的患者,在诊断时没有明确的预后因素。治疗反应的程度可能是这些患者预后的信息预测因子。用于检测传统形态学技术无法检测到的AML细胞的现代检测方法,即最小残留病(MRD),可以潜在地改善治疗反应的测量。基于这些检测结果的治疗修改将改善临床管理并最终提高治愈率,这似乎是合理的。已建立的AML MRD检测方法是基于基因异常的聚合酶链反应扩增或异常免疫表型的流式细胞术检测。残留的疾病和治疗反应可以通过这些检测以一种比传统形态学检查更加敏感和客观的方式进行测量。MRD检测的广泛应用正开始改变治疗反应和缓解的定义。MRD检测的其他临床信息用途包括检测早期复发和评估新的抗白血病药物的疗效。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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