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初发急性髓系白血病伴红系或巨核系发育异常患者对标准剂量阿糖胞苷和柔红霉素治疗反应不佳

[Poor response in patients with de novo acute myeloid leukemia and erythroblastic or megakaryocytic dysplasia to treatment with standard doses of cytosine arabinoside and daunorubicin].

作者信息

Lemez P, Gáliková J, Haas T

机构信息

Hematologicko-transfuzní oddĕlení, Nemocnice Jihlava.

出版信息

Vnitr Lek. 1999 Jun;45(6):342-6.

Abstract

Erythroid and/or megakaryocytic dysplasia (EMD) was evaluated in diagnostic bone marrow smears of 37 consecutively treated cases with de novo acute myeloid leukemia (AML) M0-M2 and M4-M5 types and three newly diagnosed cases of refractory anaemia with excess of blasts in transformation. This evaluation was possible in 38 of 40 (95%) patients and 17 cases were categorized without EMD and 21 cases with EMD. One or two cycles with 3-4 doses of daunorubicin 45 mg/m2/d and cytosine arabinoside 200 mg/m2/12 h x 14 lead to complete remission in 13 of 16 cases without EMD but only in 4 of 16 cases with EMD (p = 0.004). However, 10 of 13 patients with EMD reached complete remission with 2000 mg/m2/12 h x 10 of cytosine arabinoside plus daunorubicin. After intensive consolidations 20 patients under 65 years with EMD showed significantly worse overall survival (p = 0.017) with a median 11.5 months, while the median survival was estimated 66.8 months in 15 cases under 65 years without EMD. The proposed categorization of de novo AML patients according to the EMD seems to be useful for selection of optimal induction therapy, clinically relevant for survival and might reflect two biologic groups of AML arising in two different stages of differentiation.

摘要

在37例连续接受治疗的初发急性髓系白血病(AML)M0 - M2和M4 - M5型患者以及3例新诊断的转化型难治性贫血伴原始细胞增多症患者的诊断性骨髓涂片上评估红系和/或巨核系发育异常(EMD )。40例患者中有38例(95%)可进行此项评估,其中17例无EMD,21例有EMD。给予3 - 4剂柔红霉素45mg/m²/d和阿糖胞苷200mg/m²/12小时×14天,进行1或2个周期治疗后,16例无EMD的患者中有13例达到完全缓解,而16例有EMD的患者中只有4例达到完全缓解(p = 0.004)。然而,13例有EMD的患者中有10例使用阿糖胞苷2000mg/m²/12小时×10天加柔红霉素后达到完全缓解。强化巩固治疗后,20例65岁以下有EMD的患者总生存期明显较差(p = 0.017),中位生存期为11.5个月,而15例65岁以下无EMD的患者中位生存期估计为66.8个月。根据EMD对初发AML患者进行分类,似乎有助于选择最佳诱导治疗,对生存具有临床相关性,并且可能反映了AML在两个不同分化阶段产生的两个生物学组。

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