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首页> 外文期刊>International journal of hematology >Prognostic significance of flow cytometric residual disease, dysregulated neutrophils/monocytes, and hematogones in adult acute myeloid leukemia in first remission.
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Prognostic significance of flow cytometric residual disease, dysregulated neutrophils/monocytes, and hematogones in adult acute myeloid leukemia in first remission.

机译:首次缓解的成人急性髓细胞性白血病中流式细胞仪残留疾病,中性粒细胞/单核细胞和血红蛋白失调的预后意义。

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Fifty-one consecutive non-M3 acute myeloid leukemia (AML) patients who had achieved morphologic complete remission (mCR) after induction chemotherapy were enrolled in the present study. Three characteristics of bone marrow (BM) composition analyzed by flow cytometry were combined to determine the prognostic impact. A standardized panel of reagents was used to detect residual disease of aberrant myeloid progenitor cells (RD), identify neutrophils/monocytes with dysregulated immunophenotype (dysregulated neutro/mono) and quantify the appearance of CD34(+) B-progenitor-related cluster (hematogones) simultaneously in post-induction BM of adult AML patients. Patients who had detectable RD ≥0.2 % exhibited significantly lower median leukemia-free survival (LFS) than those who did not (13.5 vs. 48.0 months; P = 0.042). Dysregulated neutro/mono abnormalities assessed by this flow cytometric scoring system (FCSS ≥2) predicted shorter LFS (8.0 vs. 39.0 months; P = 0.008). While B-progenitor-related cluster size ≥5 % predicted improved outcome, with longer LFS (not reached vs. 13.5 months; P = 0.023) and better overall survival (not reached vs. 24.0 months; P = 0.027). The proposed RD/dysregulated neutro/mono/hematogones score showed a new risk groups with different LFS in the overall patients (P = 0.0006) as well as in the subgroup of intermediate cytogenetic risk (P = 0.001). The RD/dysregulated neutro/mono/hematogones score assessed by flow cytometry for adult AML in mCR may offer a rapid and practical risk assessment providing better refinement in risk-adapted management after induction chemotherapy.
机译:本研究纳入了51例连续的非M3急性髓性白血病(AML)患者,这些患者在诱导化疗后已达到形态完全缓解(mCR)。结合流式细胞仪分析的骨髓(BM)组成的三个特征,以确定对预后的影响。标准化的试剂组用于检测异常的骨髓祖细胞(RD)的残留疾病,鉴定免疫表型失调的中性粒细胞/单核细胞(失调的中性/单核细胞),并量化CD34(+)B祖细胞相关簇(半边形)的出现。 )同时在成人AML患者的诱导后BM中使用。 RD≥0.2%的患者的中位无白血病生存期(LFS)明显低于未检测到的患者(13.5 vs. 48.0个月; P = 0.042)。通过该流式细胞计分系统(FCSS≥2)评估的中性/单反异常失调可预测LFS缩短(8.0 vs. 39.0个月; P = 0.008)。尽管与B祖细胞相关的簇大小≥5%预测结果会改善,但LFS更长(未达到vs. 13.5个月; P = 0.023)和更好的总体生存率(未达到vs. 24.0个月; P = 0.027)。拟议的RD /中性/单/偏方评分失调显示了一个新的危险人群,其总体患者(P = 0.0006)以及中等细胞遗传学风险的亚组(P = 0.001)具有不同的LFS。通过流式细胞术评估的成人AML患者的RD /中性/单/杂七聚物的RD /失调评分可以提供快速而实用的风险评估,从而在诱导化疗后更好地调整风险适应性管理。

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