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Technical Advances in the Measurement of Residual Disease in Acute Myeloid Leukemia

机译:急性髓样白血病残留疾病检测的技术进展

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Outcomes for those diagnosed with acute myeloid leukemia (AML) remain poor. It has been widely established that persistent residual leukemic burden, often referred to as measurable or minimal residual disease (MRD), after induction therapy or at the time of hematopoietic stem cell transplant (HSCT) is highly predictive for adverse clinical outcomes and can be used to identify patients likely to experience clinically evident relapse. As a result of inherent genetic and molecular heterogeneity in AML, there is no uniform method or protocol for MRD measurement to encompass all cases. Several techniques focusing on identifying recurrent molecular and cytogenetic aberrations or leukemia-associated immunophenotypes have been described, each with their own strengths and weaknesses. Modern technologies enabling the digital quantification and tracking of individual DNA or RNA molecules, next-generation sequencing (NGS) platforms, and high-resolution imaging capabilities are among several new avenues under development to supplement or replace the current standard of flow cytometry. In this review, we outline emerging modalities positioned to enhance MRD detection and discuss factors surrounding their integration into clinical practice.
机译:对于那些诊断为急性髓细胞性白血病(AML)的患者,结果仍然很差。众所周知,诱导治疗后或造血干细胞移植(HSCT)时,持续残留的白血病负担(通常称为可测量的或最小残留的疾病(MRD))可高度预测不良的临床结果,可用于治疗以确定可能经历临床明显复发的患者。由于AML固有的遗传和分子异质性,没有统一的MRD测量方法或协议可涵盖所有情况。已经描述了几种专注于鉴定复发性分子和细胞遗传学畸变或与白血病相关的免疫表型的技术,每种技术各有优缺点。能够对单个DNA或RNA分子进行数字量化和跟踪的现代技术,下一代测序(NGS)平台和高分辨率成像功能,正在开发中以补充或替代当前流式细胞仪标准的几种新途径。在这篇综述中,我们概述了旨在增强MRD检测的新兴方法,并讨论了将其整合到临床实践中的因素。

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