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采用MOAD(一种不含蒽环类药物的方案)对成人急性淋巴细胞白血病进行治疗及潜在治愈的长期随访

Long-term follow-up of treatment and potential cure of adult acute lymphocytic leukemia with MOAD: a non-anthracycline containing regimen.

作者信息

Wiernik P H, Dutcher J P, Paietta E, Gucalp R, Markus S, Weinberg V, Azar C, Garl S, Benson L

机构信息

Albert Einstein Cancer Center, Bronx, NY.

出版信息

Leukemia. 1993 Aug;7(8):1236-41.

PMID:8350624
Abstract

A total of 55 previously untreated adults with acute lymphocytic leukemia (ALL), median age 38 years (range 15-73 years), were treated with MOAD (methotrexate, vincristine, L-asparaginase, and dexamethasone). This regimen includes five phases--induction, consolidation, cytoreduction, maintenance, and central nervous system (CNS) prophylaxis with parenteral high-dose methotrexate. Of the 55 evaluable patients, 42 achieved complete remission 76%), with a median CR duration of 12+ months (range 0.5-195+ months). The median survival in remission is 22+ months (range 1-198+ months), with 33% of remitters continuing in long-term remissions (> 5 years). Two out of four patients who developed CNS leukemia did so without marrow relapse, were successfully treated for that complication, and continue in total complete remission at 8+ and 16+ years. Another patient with extramedullary relapse (breast) was treated with radiation to that site and remains in total CR at 16+ years. Expected toxicities included myelosuppression during the induction phase of treatment, with 65% of patients requiring intravenous antibiotics. Mucositis was the next most frequent toxicity and required dose-reduction in seven patients. Minimal toxicity was seen during the post-remission phases of treatment. L-Asparaginase toxicity was more prominent during intravenous administration (24 patients) than when the intramuscular route of administration (30 patients) was used. The remission rate and long-term survivorship achieved with this regimen, without the use of an anthracycline, is comparable to that of other regimens for adult ALL. MOAD was well-tolerated by young and old adults with ALL. Aseptic necrosis of bone, successfully treated in each instance, occurred in four long-term disease-free survivors. The effect of this complication and its treatment on quality of life has been negligible.

摘要

共有55例既往未接受过治疗的急性淋巴细胞白血病(ALL)成年患者,中位年龄38岁(范围15 - 73岁),接受了MOAD(甲氨蝶呤、长春新碱、L - 天冬酰胺酶和地塞米松)治疗。该方案包括五个阶段——诱导、巩固、细胞减灭、维持以及用胃肠外高剂量甲氨蝶呤进行中枢神经系统(CNS)预防。在55例可评估患者中,42例实现完全缓解(76%),完全缓解的中位持续时间为12 + 个月(范围0.5 - 195 + 个月)。缓解期的中位生存期为22 + 个月(范围1 - 198 + 个月),33%的缓解者持续处于长期缓解状态(> 5年)。4例发生中枢神经系统白血病的患者中有2例在无骨髓复发的情况下出现,针对该并发症得到成功治疗,并且在8 + 年和16 + 年时仍处于完全缓解状态。另一名髓外复发(乳腺)患者接受了该部位的放疗,在16 + 年时仍处于完全缓解状态。预期的毒性包括治疗诱导期的骨髓抑制,65%的患者需要静脉使用抗生素。粘膜炎是其次最常见的毒性反应,7例患者需要减少剂量。缓解期治疗阶段毒性反应轻微。L - 天冬酰胺酶静脉给药(24例患者)时的毒性比肌肉注射给药(30例患者)时更明显。该方案在未使用蒽环类药物的情况下所达到的缓解率和长期生存率与其他成人ALL方案相当。ALL的年轻和老年患者对MOAD耐受性良好。4例长期无病生存者发生了骨无菌性坏死,每次均成功治疗。该并发症及其治疗对生活质量的影响可忽略不计。

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