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Minimal residual disease in multiple myeloma: defining the role of next generation sequencing and flow cytometry in routine diagnostic use

机译:多发性骨髓瘤中的最小残留疾病:定义下一代测序和流式细胞术在常规诊断使用中的作用

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摘要

For patients diagnosed with multiple myeloma (MM) there have been significant treatment advances over the past decade, reflected in an increasing proportion of patients achieving durable remissions. Clinical trials repeatedly demonstrate that achieving a deep response to therapy, with a bone marrow assessment proving negative for minimal residual disease (MRD), confers a significant survival advantage. To accurately assess for minute quantities of residual cancer requires highly sensitive methods; either multiparameter flow cytometry or next generation sequencing are currently recommended for MM response assessment. Under optimal conditions, these methods can detect one aberrant cell amongst 1,000,000 normal cells (a sensitivity of 10-6). Here, we will review the practical use of MRD assays in MM, including challenges in implementation for the routine diagnostic laboratory, standardisation across laboratories and clinical trials, the clinical integration of MRD status assessment into MM management and future directions for ongoing research.
机译:对于诊断为多发性骨髓瘤(MM)的患者,在过去十年中有了显著的治疗进展,这反映在获得持久缓解的患者比例不断增加。临床试验反复证明,获得对治疗的深度反应,骨髓评估证明最小残留病(MRD)为阴性,这将带来显著的生存优势。要准确评估微小残留癌症数量,需要高度敏感的方法;目前推荐使用多参数流式细胞术或下一代测序来评估MM反应。在最佳条件下,这些方法可以检测1000000个正常细胞中的一个异常细胞(灵敏度为10-6)。在这里,我们将回顾MRD分析在MM中的实际应用,包括常规诊断实验室实施中的挑战、实验室和临床试验的标准化、MRD状态评估与MM管理的临床整合,以及正在进行的研究的未来方向。

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