通过多参数流式细胞术确定的可测量残留疾病与成年急性白血病患者临床复发的中等风险有关

IF 3.6 3区 医学 Q1 PATHOLOGY
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引用次数: 0

摘要

可测量残留病(MRD)有助于预后和监测急性白血病患者对治疗的反应。多参数流式细胞术(MFC-MRD)利用白血病相关免疫表型(LAIP)和与正常细胞的差异(DfN)策略来确定白血病克隆。当 LAIP 与正常再生重叠、出现克隆进化或异常克隆数量极少(如 CD45 细胞小于 0.01%)时,就会出现困难。此类病例被报告为 "不确定 "病例;然而,国际上对此报告几乎没有共识。临床结果与 MFC-MRD 不确定性之间的关系尚不清楚。在此,我们确定了MFC-MRD报告的不确定率、其与同期分子MRD结果(如有)的关系,以及与12个月临床结果的关系。我们对 2021 年 1 月至 12 月间所有成人的 MFC-MRD 检测进行了内部审计。共纳入了 153 名诊断为急性白血病的连续患者。自纳入研究起,在12个月内记录了连续的MFC-MRD结果和临床结果。共审查了 153 名患者的 460 次 MFC-MRD 检测结果,54 名患者(35%)的 73 次(16%)MFC-MRD 检测结果被报告为不确定。大多数(70%)患者的 CD45 细胞水平较低,在 0.01-0.1% 之间。与结果为阴性的患者相比,MFC-MRD不确定的患者中急性髓性白血病(AML)的发病率更高(70% 对 36%),而 B 细胞急性淋巴细胞白血病的发病率较低(20% 对 55%)。在MFC-MRD结果不确定的患者中,有三分之一的人在此前3个月内接受过化疗或异体造血干细胞移植(aHSCT)。MFC和分子MRD检测之间的一致性较低。MFC-MRD不确定患者的白血病复发率低于MFC-MRD阳性患者,但高于MFC-MRD阴性患者(阳性33% vs 不确定21% vs 阴性8%,=0.038)。总之,这些研究结果表明,MFC-MRD结果不确定在成人急性髓细胞性白血病患者中更为常见,在前3个月内接受过化疗或aHSCT的患者中也更为常见。我们首次报告了MFC-MRD不确定结果具有潜在的临床意义,与MFC-MRD阴性结果相比,它与12个月内中位复发率较高有关。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Indeterminate measurable residual disease by multiparameter flow cytometry is associated with an intermediate risk of clinical relapse in adult patients with acute leukaemia

Measurable residual disease (MRD) is useful for prognostication and for monitoring response to treatment in patients with acute leukaemia. MRD by multiparametric flow cytometry (MFC-MRD) utilises the leukaemia-associated immunophenotype (LAIP) and difference from normal (DfN) strategies to identify the leukaemic clone. Difficulties arise when the LAIP overlaps with normal regeneration, there is clonal evolution, or when the abnormal clone population is exceptionally small e.g., <0.01% of CD45+ cells. Such cases are reported as ‘indeterminate’; however, there is little international consensus on this reporting. The relationship between clinical outcomes and indeterminate MFC-MRD is unknown. Here we determine the rate of indeterminate MFC-MRD reporting, its relationship to concurrent molecular MRD results when available, and to clinical outcomes to 12 months. We performed an internal audit of all adult testing for MFC-MRD between January and December 2021. A total of 153 consecutive patients with a diagnosis of acute leukaemia were included. Successive MFC-MRD results and clinical outcomes were recorded over a 12-month period from time of inclusion into the study. In total, 460 MFC-MRD tests from 153 patients were reviewed and 73 (16%) MFC-MRD tests from 54 (35%) patients were reported as indeterminate. The majority (70%) were at low levels between 0.01–0.1% of CD45+ cells. Compared to patients with a negative result, acute myeloid leukaemia (AML) was more frequent in patients who had an indeterminate MFC-MRD (70% vs 36%), and B-cell acute lymphoblastic leukaemia was less common (20% vs 55%). In patients with indeterminate MFC-MRD results, one-third had received either chemotherapy or allogeneic haemopoietic stem cell transplant (aHSCT) within the preceding 3 months. Agreement between MFC and molecular MRD testing was low. Patients with indeterminate MFC-MRD had leukaemia relapse rates below patients with a positive MFC-MRD, but greater than those with negative MFC-MRD (positive 33% vs indeterminate 21% vs negative 8%, p = 0.038). Overall, these findings indicate that indeterminate MFC-MRD results are more common in adults with AML and also in those who have received chemotherapy or aHSCT within the previous 3 months. We report for the first time that indeterminate MFC-MRD is a finding of potential clinical significance, which associates with a numerically higher median relapse rate within 12 months when compared to a negative MFC-MRD result.

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来源期刊
Pathology
Pathology 医学-病理学
CiteScore
6.50
自引率
2.20%
发文量
459
审稿时长
54 days
期刊介绍: Published by Elsevier from 2016 Pathology is the official journal of the Royal College of Pathologists of Australasia (RCPA). It is committed to publishing peer-reviewed, original articles related to the science of pathology in its broadest sense, including anatomical pathology, chemical pathology and biochemistry, cytopathology, experimental pathology, forensic pathology and morbid anatomy, genetics, haematology, immunology and immunopathology, microbiology and molecular pathology.
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