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颅脑照射能否降低急性髓系白血病骨髓复发的风险?儿童急性髓系白血病研究BFM - 87的意外结果。

Does cranial irradiation reduce the risk for bone marrow relapse in acute myelogenous leukemia? Unexpected results of the Childhood Acute Myelogenous Leukemia Study BFM-87.

作者信息

Creutzig U, Ritter J, Zimmermann M, Schellong G

机构信息

University Children's Hospital, Münster, Germany.

出版信息

J Clin Oncol. 1993 Feb;11(2):279-86. doi: 10.1200/JCO.1993.11.2.279.

Abstract

PURPOSE

One of the goals of study AMA-BFM-87 was to test prospectively in acute myelogenous leukemia (AML) patients if cranial irradiation could be replaced by late intensification therapy with high-dose cytarabine (Ara-C) and etoposide (VP-16).

PATIENTS AND METHODS

Patients with a low risk of CNS relapses (ie, no initial CNS disease, WBC count at diagnosis < or = 70.000/microL) were randomized for irradiation (group A, 31 patients). In 25 patients (group B), randomization was refused. As interim results showed no increase of CNS relapses in nonirradiated patients, prophylactic irradiation was discontinued after 2 1/2 years to prevent unnecessary CNS toxicity. Forty-four patients (group C) entered the study after randomization had been stopped.

RESULTS

In all patients with a low risk of CNS recurrences (n = 100), a significantly higher probability of relapse-free interval (pRFI) of 5 years was found in irradiated patients (pRFI = .78) compared with nonirradiated patients (pRFI = .41) (P = .007). Moreover, a slightly higher incidence of CNS relapses was observed in nonirradiated patients. Due to the small number of patients, this was not observed when randomized patients only were analyzed. In accordance with these findings, the favorable outcome of low-risk patients in the preceding study, AML-BFM-83 (pRFI > .80), could only be reproduced in study AML-BFM-87 in patients who had received cranial irradiation.

CONCLUSION

These results indicate that cranial irradiation should be an integral part of the treatment of all AML patients not undergoing bone marrow transplantation. Residual blasts in the CNS may escape systemic chemotherapy and lead to recurrence of the initial disease not only in the CNS, but also in the bone marrow.

摘要

目的

研究AMA - BFM - 87的目标之一是前瞻性地测试在急性髓性白血病(AML)患者中,高剂量阿糖胞苷(Ara - C)和依托泊苷(VP - 16)的晚期强化治疗是否可以替代颅脑照射。

患者与方法

中枢神经系统(CNS)复发风险低(即初始无CNS疾病,诊断时白细胞计数≤70,000/μL)的患者被随机分为接受照射组(A组,31例患者)。25例患者(B组)拒绝随机分组。由于中期结果显示未接受照射的患者CNS复发率未增加,2年半后停止预防性照射以防止不必要的CNS毒性。随机分组停止后,44例患者(C组)进入研究。

结果

在所有CNS复发风险低的患者(n = 100)中,与未接受照射的患者相比,接受照射的患者5年无复发生存期(pRFI)显著更高(pRFI = 0.78),未接受照射的患者pRFI = 0.41(P = 0.007)。此外,未接受照射的患者中CNS复发率略高。由于患者数量较少,仅分析随机分组的患者时未观察到这一点。根据这些发现,在前一项研究AML - BFM - 83中低风险患者的良好结局(pRFI>0.80),仅在接受颅脑照射的AML - BFM - 87研究患者中得以重现。

结论

这些结果表明,颅脑照射应成为所有未接受骨髓移植的AML患者治疗的一个组成部分。CNS中的残留原始细胞可能逃避全身化疗,不仅导致初始疾病在CNS复发,还会在骨髓复发。

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