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Prognostic Relevance of Cytokine Receptor Expression in Acute Myeloid Leukemia: Interleukin-2 Receptor α-Chain (CD25) Expression Predicts a Poor Prognosis

机译:细胞因子受体表达在急性髓性白血病中的预后相关性:白细胞介素2受体α链(CD25)表达预测不良的预后。

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摘要

A variety of cytokine/cytokine receptor systems affect the biological behavior of acute leukemia cells. However, little is known about the clinical relevance of cytokine receptor expression in acute myeloid leukemia (AML). We quantitatively examined the expression of interleukin-2 receptor α-chain (IL-2Rα, also known as CD25), IL-2Rβ, IL-3Rα, IL-4Rα, IL-5Rα, IL-6Rα, IL-7Rα, the common β-chain (βc), γc, granulocyte-macrophage colony-stimulating factor (GM-CSF)Rα, G-CSFR, c-fms, c-mpl, c-kit, FLT3, and GP130 in leukemia cells from 767 adult patients with AML by flow cytometry and determined their prevalence and clinical significance. All cytokine receptors examined were expressed at varying levels, whereas the levels of IL-3Rα, GM-CSFRα, IL-2Rα, γc, c-kit, and G-CSFR exhibited a wide spectrum of ≥10,000 sites/cell. In terms of their French-American-British classification types, GM-CSFRα and c-fms were preferentially expressed in M4/M5 patients, G-CSF in M3 patients, and IL-2Rα in non-M3 patients. Elevated levels of IL-3Rα, GM-CSFRα, and IL-2Rα correlated with leukocytosis. In patients ≤60 years old, higher levels of these 3 receptors correlated with poor responses to conventional chemotherapy, but only IL-2Rα was associated with a shorter overall survival. By incorporating IL-2Rα status into cytogenetic risk stratification, we could sort out a significantly adverse-risk cohort from the cytogenetically intermediate-risk group. Analyses with various phenotypical risk markers revealed the expression of IL-2Rα as an independent prognostic indicator in patients with intermediate-risk cytogenetics. These findings were not observed in patients >60 years old. Our results indicate that several cytokine receptors were associated with certain cellular and clinical features, but IL-2Rα alone had prognostic value that provides an additional marker to improve current risk evaluation in AML patients ≤60 years old.
机译:多种细胞因子/细胞因子受体系统影响急性白血病细胞的生物学行为。但是,关于急性髓细胞白血病(AML)中细胞因子受体表达的临床相关性知之甚少。我们定量检查了白介素2受体α链(IL-2Rα,也称为CD25),IL-2Rβ,IL-3Rα,IL-4Rα,IL-5Rα,IL-6Rα,IL-7Rα的表达。 767名成年患者白血病细胞中的β链(βc),γc,粒细胞巨噬细胞集落刺激因子(GM-CSF)Rα,G-CSFR,c-fms,c-mpl,c-kit,FLT3和GP130流式细胞仪检测AML的患病率并确定其临床意义。检查的所有细胞因子受体均以不同的水平表达,而IL-3Rα,GM-CSFRα,IL-2Rα,γc,c-kit和G-CSFR的水平显示≥10,000个位点/细胞的广谱。就法国-美国-英国分类类型而言,M4 / M5患者中优先表达GM-CSFRα和c-fms,M3患者中优先表达G-CSF,非M3患者中优先表达IL-2Rα。 IL-3Rα,GM-CSFRα和IL-2Rα的升高与白细胞增多有关。在≤60岁的患者中,这三种受体的水平较高与对常规化学疗法的不良反应有关,但只有IL-2Rα与较短的总生存期有关。通过将IL-2Rα状态纳入细胞遗传学风险分层中,我们可以从细胞遗传学中度风险组中筛选出明显的不良风险队列。对各种表型危险因素的分析表明,IL-2Rα的表达是中危细胞遗传学患者的独立预后指标。在> 60岁的患者中未观察到这些发现。我们的结果表明,几种细胞因子受体与某些细胞和临床特征有关,但单独的IL-2Rα具有预后价值,可提供另外的标志物来改善60岁以下AML患者的当前风险评估。

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