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The number of CD34+CD38+CD117+HLA-DR+CD13+CD33+ cells indicates post-chemotherapy hematopoietic recovery in patients with acute myeloid leukemia

机译:CD34 + CD38 + CD117 + HLA-DR + CD13 + CD33 +细胞的数量表明急性髓细胞白血病患者化疗后的造血功能恢复

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摘要

Hematopoietic recovery is considered to be associated with the number of multipotent hematopoietic stem cells in the bone marrow, as observed in functional assays involving stem cell transplantation. However, there is little evidence related to hematopoietic recovery in non-transplantation settings, which is accomplished by endogenous hematopoietic cells. A recent study suggested that progenitors are the main contributors during this steady-state hematopoiesis, which differs from exogenous transplantation. We hypothesized that endogenous progenitor support post-chemotherapy hematopoietic recovery. To investigate the potential impact of these progenitor cell percentage on hematopoietic recovery, we retrospectively analyzed the percentage of CD34+CD38+CD117+HLA-DR+CD13+CD33+ cells (P cells) and hematopoietic recovery in 223 newly diagnosed acute myeloid leukemia patients during two courses of consolidation chemotherapy after complete remission. We found that a lower P cell percentage was significantly associated with prolonged neutropenia recovery time after the first and second courses of consolidation chemotherapy (p = 0.001; p = 0.045, respectively). We also observed similar results with regard to platelet recovery time after the first course of consolidation chemotherapy (p = 0.000). Univariate analysis showed that P cell percentage and consolidation chemotherapy regimens, and not gender, age, induction chemotherapy regimens, infection grade, WHO classification and NCCN risk category, were associated with neutrophil recovery after chemotherapy. Multivariate analysis demonstrated that P cell percentage is an independent factor affecting neutrophil recovery capacity for both the first and second courses (p = 0.008; p = 0.032, respectively). Our results indicate that CD34+CD38+CD117+HLA-DR+CD13+CD33+ cells before each course of chemotherapy is independently associated with chemotherapy-related hematopoietic reconstitution capacity. These findings may help modify future chemotherapy regimens based on progenitor cell percentages.
机译:如涉及干细胞移植的功能测定中所观察到的,造血功能恢复与骨髓中多能造血干细胞的数量有关。但是,很少有证据表明在非移植环境中造血功能恢复是由内源性造血细胞完成的。最近的一项研究表明,祖细胞是这种稳态造血过程的主要贡献者,这与外源性移植不同。我们假设内源性祖细胞支持化疗后的造血功能恢复。为了调查这些祖细胞百分比对造血功能恢复的潜在影响,我们回顾性分析了223例新诊断的急性髓细胞性白血病患者中CD34 + CD38 + CD117 + HLA-DR + CD13 + CD33 +细胞(P细胞)的百分比和造血功能恢复。完全缓解后进行两个疗程的巩固化疗。我们发现,在合并化疗的第一和第二疗程后,较低的P细胞百分比与中性粒细胞减少的恢复时间延长显着相关(分别为p = 0.001; p = 0.045)。我们也观察到在巩固化疗的第一个疗程后血小板恢复时间方面的相似结果(p = 0.000)。单因素分析显示,P细胞百分比和巩固化疗方案与性别,年龄,诱导化疗方案,感染等级,WHO分类和NCCN风险类别无关,而与化疗后中性粒细胞的恢复有关。多变量分析表明,P细胞百分比是影响第一个疗程和第二个疗程的中性粒细胞恢复能力的独立因素(分别为p = 0.008; p = 0.032)。我们的结果表明,在每个疗程之前,CD34 + CD38 + CD117 + HLA-DR + CD13 + CD33 +细胞与化疗相关的造血重建能力独立相关。这些发现可能有助于基于祖细胞百分比修改未来的化疗方案。

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