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复发急性淋巴细胞白血病患儿低剂量聚乙二醇化天冬酰胺酶(昂卡司帕)的药物监测

Drug monitoring of low-dose PEG-asparaginase (Oncaspar) in children with relapsed acute lymphoblastic leukaemia.

作者信息

Vieira Pinheiro J P, Müller H J, Schwabe D, Gunkel M, Casimiro da Palma J, Henze G, von Schütz V, Winkelhorst M, Würthwein G, Boos J

机构信息

Department of Paediatrics, University of Münster, Germany.

出版信息

Br J Haematol. 2001 Apr;113(1):115-9. doi: 10.1046/j.1365-2141.2001.02680.x.

Abstract

Use of asparaginase (ASNase) in the treatment of relapsed childhood acute lymphoblastic leukaemia (ALL) is associated with a high rate of hypersensitive reactions. 'Silent' inactivation may additionally reduce treatment intensity. Therefore, PEG-ASNase (Oncaspar), a polyethylene glycol conjugate of the native Escherichia coli-ASNase, was introduced into the Berlin-Frankfurt-Münster (BFM) 96 treatment protocol for relapsed ALL under drug monitoring conditions. A single i.v. dose of 500 IU/m2 PEG-ASNase, substituted for the native ASNases, was administered to supply a plasma activity of 100 IU/l for 1 week. From November 1997 to March 2000, 35 patients from 23 BFM-associated hospitals, with or without a previous allergic reaction to one or both native preparations, underwent monitoring. After 82 applications, a total of 270 samples were submitted to be tested for ASNase activity. The ASNase activity on the day of the administration and the following day ranged between < 20 and 693 IU/l, with a median of 413 IU/l (53 samples). The median on d 7 +/- 1 was 199 IU/l (range <20--421 IU/l; 41 samples) and on d 14 +/- 1, 105 IU/l (range <20--188 IU/l; 19 samples). An ASNase activity of > 100 IU/l was seen on d 7 in 36 activity time courses of 52 interpretable applications (69%). Intraindividual variability of activity time courses was low. However, a rapid decrease in ASNase activity after repeated applications was observed in 4 out of 20 children. Previously experienced allergic reactions to native ASNases did not influence PEG-ASNase pharmacokinetics. PEG-ASNase is a useful alternative to the native ASNases in children with relapsed ALL. Whenever possible, drug monitoring should be performed to identify patients with 'silent' inactivation.

摘要

天冬酰胺酶(ASNase)用于治疗复发性儿童急性淋巴细胞白血病(ALL)时,过敏反应发生率很高。“沉默”失活可能还会降低治疗强度。因此,聚乙二醇化天冬酰胺酶(Oncaspar),即天然大肠杆菌天冬酰胺酶的聚乙二醇共轭物,在药物监测条件下被引入柏林-法兰克福-明斯特(BFM)96复发性ALL治疗方案中。静脉注射单剂量500 IU/m²聚乙二醇化天冬酰胺酶,替代天然天冬酰胺酶,给药后可使血浆活性维持在100 IU/l达1周。1997年11月至2000年3月,来自23家与BFM相关医院的35例患者,无论之前是否对一种或两种天然制剂有过敏反应,均接受了监测。82次用药后,共提交了270份样本检测天冬酰胺酶活性。给药当天及次日的天冬酰胺酶活性在<20至693 IU/l之间,中位数为413 IU/l(53份样本)。第7±1天的中位数为199 IU/l(范围<20-421 IU/l;41份样本),第14±1天为105 IU/l(范围<20-188 IU/l;19份样本)。在52次可解释用药的36次活性时间进程中,第7天观察到天冬酰胺酶活性>100 IU/l(69%)。活性时间进程的个体内变异性较低。然而,20名儿童中有4名在重复用药后观察到天冬酰胺酶活性迅速下降。既往对天然天冬酰胺酶的过敏反应不影响聚乙二醇化天冬酰胺酶的药代动力学。聚乙二醇化天冬酰胺酶是复发性ALL儿童患者中天然天冬酰胺酶的有用替代物。只要有可能,就应进行药物监测以识别“沉默”失活的患者。

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