6-巯基嘌呤在儿童急性淋巴细胞白血病中的耐受性
[Tolerability of 6-mercaptopurine in children with acute lymphoblastic leukemia].
作者信息
Ma Xiao-li, Wang Bin, Guo Hai-ying, Zhang Yong-hong, Zhu Guang-hua, Duan Yan-long, Yang Jing, Zhang Da-wei, Jin Ling, Zhang Rui, Zhang Li, Xie Jin, Wu Min-yuan
机构信息
Hematology Center, Beijing Children's Hospital, Capital Medical University, Beijing 100045, China.
出版信息
Zhonghua Er Ke Za Zhi. 2010 Apr;48(4):289-92.
OBJECTIVE
6-Mercaptopurine (6-MP) has been the backbone of maintenance chemotherapy for acute lymphoblastic leukemia (ALL), the response to 6-MP is highly variable, adverse events leading to discontinuation or dose-reduction (children intolerant) of 6-MP occur in many children with ALL. The aim of this study was to investigate the tolerability of 6-MP and to optimize thiopurine use.
METHODS
The authors evaluated in a prospective manner the tolerance of 6-MP in ALL children from Oct. 1, 2004 to Sept. 30, 2007 who were newly diagnosed in Beijing Children's Hospital, using BCH-ALL-2003 protocols, during the maintenance therapy and followed up to Sept. 30, 2008. All children had a treatment period of at least 3 months for maintenance therapy.
RESULTS
Totally 133 children including 81 boys and 52 girls at median age of 67 months (18 - 188 months), 100% of the patients went into complete remission (CR) on day 33 of induction chemotherapy, and the median time to CR was 26 months (6 - 47 months). All the children had maintenance therapy from 3 to 25 months (mean 13.5 +/- 7.4) and 72(54%) received 6-MP standard doses continuously for total courses, the median daily dose of 6-MP was 46 mg/(m(2).d) 6-MP, their WBC was (3 - 4) x 10(9)/L, ANC (1.5 - 2) x 10(9)/L, they had no severe liver toxicity. In 4 children the dose of 6-MP was increased to 125% because WBC was higher than 6 x 10(9)/L, ANC higher than 3 x 10(9)/L. Sixty one children (46%) had poor tolerability to 6-MP, they experienced adverse events that led to discontinuation (n = 19) or dose reduction (n = 42) of 6-MP, the actual mean dose for the 42 cases was 25 - 30 mg/(m(2).d) and the time to occurrence of toxic effects was 2.5 weeks. Reasons for discontinuation or dose reduction were severe myelotoxicity occurred in 48 children, hepatotoxicity in 12, and skin rash in one.
CONCLUSIONS
In this cohort of ALL children, the difference of tolerance to oral 6-MP was obvious, 54% of the children well tolerated 6-MP during the whole course at oral standard dose, and severe granulocytopenia did not occur. However, 46% developed severe granulopenia or hepatotoxicity, the dosage had to be reduced in order to decrease the probability of severe toxicity. It is suggested that standard dose of 6-MP is not always the maximum tolerant dose in some children and inadequate dose may be the cause of therapy failure.
目的
6-巯基嘌呤(6-MP)一直是急性淋巴细胞白血病(ALL)维持化疗的主要药物,但对6-MP的反应差异很大,许多ALL患儿会出现导致6-MP停药或减量(儿童不耐受)的不良事件。本研究旨在调查6-MP的耐受性并优化硫嘌呤的使用。
方法
作者前瞻性评估了2004年10月1日至2007年9月30日在北京儿童医院新诊断的ALL患儿使用BCH-ALL-2003方案进行维持治疗并随访至2008年9月30日期间6-MP的耐受性。所有患儿维持治疗期至少3个月。
结果
共133例患儿,其中男81例,女52例,中位年龄67个月(18 - 188个月),100%的患者在诱导化疗第33天达到完全缓解(CR),CR的中位时间为26个月(6 - 47个月)。所有患儿维持治疗3至25个月(平均13.5±7.4),72例(54%)全程接受6-MP标准剂量,6-MP的中位日剂量为46mg/(m²·d),其白细胞计数为(3 - 4)×10⁹/L,中性粒细胞绝对值计数为(1.5 - 2)×10⁹/L,无严重肝毒性。4例患儿因白细胞高于6×10⁹/L、中性粒细胞绝对值计数高于3×10⁹/L,6-MP剂量增至125%。61例患儿(46%)对6-MP耐受性差,出现导致6-MP停药(19例)或减量(42例)的不良事件,42例实际平均剂量为25 - 30mg/(m²·d),毒性效应出现时间为2.5周。停药或减量的原因是48例发生严重骨髓毒性,12例发生肝毒性,1例发生皮疹。
结论
在这组ALL患儿中,口服6-MP的耐受性差异明显,54%的患儿在口服标准剂量全程中对6-MP耐受性良好,未发生严重粒细胞减少。然而,46%的患儿出现严重粒细胞减少或肝毒性,必须减量以降低严重毒性的发生概率。提示6-MP标准剂量在部分患儿中并非总是最大耐受剂量,剂量不足可能是治疗失败的原因。
Zotero 插件