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儿童白血病中的细胞耐药性。

Cellular drug resistance in childhood leukemia.

作者信息

Veerman A J, Kaspers G J, Pieters R

机构信息

Department of Pediatrics, Free University Hospital, Amsterdam, The Netherlands.

出版信息

Ann Hematol. 1994;69 Suppl 1:S31-4. doi: 10.1007/BF01757352.

Abstract

The response to chemotherapy is determined essentially by two factors: first, pharmacokinetic factors, determining which concentration of drug reaches the malignant cells, and second, cellular drug resistance of these cells, determining how many of them will be killed by that concentration of drug. The study of cellular drug resistance has been stimulated by the development of short-term 'total cell kill' assays, such as the MTT assay, for use on patient samples. The drug resistance profiles differed markedly between ALL and ANLL, between immunophenotypic and karyotypic subgroups within ALL, and between initial and relapsed ALL. The results of the MTT assay showed a significant relation between the antileukemic activity of prednisolone in vitro and the clinical response to systemic monotherapy with that drug. At multivariate analysis including several well-known prognostic factors (WBC, age, immunophenotype) only the in vitro resistance to prednisolone, dexamethasone, L-asparaginase, and daunorubicin was significantly related to clinical outcome. At multiple regression analysis, combination of the results for prednisolone, L-asparaginase, and vincristine made it possible to distinguish between three patient groups with increasing levels of drug resistance and markedly different probabilities of 2-year disease-free survival: 100%, 83%, and 60%. These results show that in vitro drug resistance testing can give a correct prediction of prognosis, superior to that of currently used prognostic factors. Stratification of prognostic groups based on the results of drug resistance testing is feasible and should be introduced into new clinical trials. Many questions now remaining could be answered within carefully designed preclinical and clinical studies.

摘要

化疗反应基本上由两个因素决定

其一,药代动力学因素,它决定了何种浓度的药物能够到达恶性细胞;其二,这些细胞的细胞耐药性,它决定了在该药物浓度下有多少细胞会被杀死。短期“全细胞杀伤”检测方法(如MTT检测法)的发展推动了对细胞耐药性的研究,这些检测方法可用于患者样本。急性淋巴细胞白血病(ALL)和急性非淋巴细胞白血病(ANLL)之间、ALL内免疫表型和核型亚组之间以及初发ALL和复发ALL之间的耐药谱存在显著差异。MTT检测结果显示,泼尼松龙的体外抗白血病活性与该药物全身单药治疗的临床反应之间存在显著关联。在包括几个知名预后因素(白细胞计数、年龄、免疫表型)的多变量分析中,只有对泼尼松龙、地塞米松、L-天冬酰胺酶和柔红霉素的体外耐药性与临床结局显著相关。在多元回归分析中,结合泼尼松龙、L-天冬酰胺酶和长春新碱的检测结果,可以区分出三组耐药水平不断升高且2年无病生存率概率明显不同的患者:100%、83%和60%。这些结果表明,体外耐药性检测能够正确预测预后,优于目前使用的预后因素。基于耐药性检测结果对预后组进行分层是可行的,应引入新的临床试验。现在许多遗留的问题可以在精心设计的临床前和临床研究中得到解答。

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