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全反式维甲酸与大剂量化疗联合治疗高白细胞急性早幼粒细胞白血病合并严重内脏出血患者。

Combined therapy with all-trans-retinoic acid and high-dose chemotherapy in patients with hyperleukocytic acute promyelocytic leukemia and severe visceral hemorrhage.

作者信息

Dombret H, Sutton L, Duarte M, Daniel M T, Leblond V, Castaigne S, Degos L

机构信息

Service Clinique des Maladies du Sang, Hospital Saint-Louis, Paris, France.

出版信息

Leukemia. 1992 Dec;6(12):1237-42.

PMID:1453767
Abstract

Acute promyelocytic leukemia (APL) is associated with a high incidence of disseminated intravascular coagulation (DIC) and early hemorrhagic death. The risk of early fatal hemorrhage is increased when high peripheral-blood blast count and severe DIC accompanied by visceral hemorrhage are present at diagnosis. Progressive cytolysis induced by daily increased doses of chemotherapy, or differentiation all-trans-retinoic acid (ATRA) therapy have been proposed for initial control of DIC, but both are dangerous in hyperleukocytic APL patients. We report our results obtained in three high-risk APL patients treated with a combination of conventional chemotherapy and ATRA. All patients had documented hyperleukocytic APL [M3 or M3-variant subtype, (15, 17) translocation] with DIC, and all had critical clinical course before treatment. Patient 1 presented with cerebral hemorrhage, patients 2 and 3 had acute respiratory failure probably due to pulmonary leukemic infiltration and pulmonary hemorrhage. In order to minimize the severity of DIC during chemotherapy-induced acute cytolysis, ATRA (45 mg/m2 per day) was started on the first or second day of chemotherapy and withdrawn when complete remission (CR) was achieved. Despite adverse clinical features, CR was obtained in these three high-risk patients. Patient 1 showed no increase of cerebral bleeding during therapy. Patients 2 and 3 required transient intensive care, with mechanical ventilation from day 4 to day 11 for one of them. Differentiating granular cells were present in peripheral blood of all patients from the day 5, 12 and 8 of cytotoxic therapy. For the three patients, the number of days with white blood cell count < 1 x 10(9)/l was only 2, 7 and 11 days respectively. These results suggest that differentiation therapy with ATRA may be useful even in hyperleukocytic APL patients, when ATRA is used in combination with chemotherapy. The mechanisms of this putative beneficial effect are discussed.

摘要

急性早幼粒细胞白血病(APL)与弥散性血管内凝血(DIC)的高发生率及早期出血性死亡相关。诊断时若外周血原始细胞计数高且伴有严重DIC及内脏出血,则早期致命性出血的风险会增加。有人提出通过每日增加化疗剂量诱导进行性细胞溶解或采用全反式维甲酸(ATRA)分化疗法来初步控制DIC,但这两种方法对于高白细胞性APL患者均有危险。我们报告了对3例高危APL患者采用传统化疗与ATRA联合治疗的结果。所有患者均确诊为伴有DIC的高白细胞性APL[M3或M3变异亚型,(15,17)易位],且治疗前临床过程均危急。患者1出现脑出血,患者2和3出现急性呼吸衰竭,可能是由于肺部白血病浸润和肺出血所致。为了在化疗诱导的急性细胞溶解过程中将DIC的严重程度降至最低,在化疗的第1天或第2天开始使用ATRA(每天45mg/m²),在达到完全缓解(CR)时停药。尽管有不良临床特征,但这3例高危患者均获得了CR。患者1在治疗期间脑出血未加重。患者2和3需要短暂的重症监护,其中1例从第4天至第11天需要机械通气。从细胞毒性治疗的第5天、12天和8天起,所有患者外周血中均出现了分化的粒细胞。对于这3例患者,白细胞计数<1×10⁹/L的天数分别仅为2天、7天和11天。这些结果表明,如果将ATRA与化疗联合使用,即使对于高白细胞性APL患者,分化疗法可能也是有效的。本文讨论了这种假定有益作用的机制。

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