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儿童急性淋巴细胞白血病中的泼尼松龙耐药性:体外-体内相关性及对其他药物的交叉耐药性。

Prednisolone resistance in childhood acute lymphoblastic leukemia: vitro-vivo correlations and cross-resistance to other drugs.

作者信息

Kaspers G J, Pieters R, Van Zantwijk C H, Van Wering E R, Van Der Does-Van Den Berg A, Veerman A J

机构信息

Department of Pediatric Hematology/Oncology, University Hospital Vrije Universiteit, Amsterdam, The Netherlands.

出版信息

Blood. 1998 Jul 1;92(1):259-66.

PMID:9639525
Abstract

As an important determinant of response to chemotherapy, accurate measurement of cellular drug resistance may provide clinically relevant information. Our objectives in this study were to determine the relationship between in vitro resistance to prednisolone (PRD) measured with the colorimetric methyl-thiazol-tetrazolium (MTT) assay, and (1) short-term clinical response to systemic PRD monotherapy, (2) long-term clinical outcome after combination chemotherapy within all patients and within the subgroups of clinical good and poor responders to PRD, and (3) in vitro resistance to 12 other drugs in 166 children with newly diagnosed acute lymphoblastic leukemia (ALL). The 12 clinical poor PRD responders had ALL cells that were median 88-fold more in vitro resistant to PRD than 131 good responders (P = .013). Within all patients, increased in vitro resistance to PRD predicted a significantly worse long-term clinical outcome, at analyses with and without stratification for clinical PRD response, and at multivariate analysis (P </= .001). Within both the clinical good and poor responder subgroups, increased in vitro resistance to PRD was associated with a worse outcome, which was significant within the group of clinical good responders (P < .001). LC50 values, ie, lethal concentrations to 50% of ALL cells, for PRD and each other drug correlated significantly with those of all other 12 drugs, with an average correlation coefficient of 0.44 (standard deviation 0.05). The highest correlations were found between structurally related drugs. In conclusion, in vitro resistance to PRD was significantly related to the short-term and long-term clinical response to chemotherapy, the latter also within the subgroup of clinical good responders to PRD. There was a more general in vitro cross-resistance between anticancer drugs in childhood ALL, although drug-specific activities were recognized.

摘要

作为化疗反应的一个重要决定因素,准确测量细胞耐药性可为临床提供相关信息。我们这项研究的目的是确定用比色法甲基噻唑四氮唑(MTT)测定的体外对泼尼松龙(PRD)的耐药性与以下因素之间的关系:(1)系统性PRD单一疗法的短期临床反应;(2)联合化疗后所有患者以及PRD临床反应良好和不良亚组的长期临床结局;(3)166例新诊断的急性淋巴细胞白血病(ALL)患儿对其他12种药物的体外耐药性。12例临床PRD反应不良者的ALL细胞对PRD的体外耐药性比131例反应良好者的细胞中位数高88倍(P = 0.013)。在所有患者中,体外对PRD耐药性增加预示着长期临床结局显著更差,无论是否对临床PRD反应进行分层分析以及多变量分析时均如此(P≤0.001)。在临床反应良好和不良亚组中,体外对PRD耐药性增加均与更差的结局相关,在临床反应良好的亚组中这种相关性具有显著性(P < 0.001)。PRD及其他每种药物的半数致死浓度(LC50)值,即对50%的ALL细胞具有致死性的浓度,与其他所有12种药物的LC50值显著相关,平均相关系数为0.44(标准差0.05)。在结构相关的药物之间发现了最高的相关性。总之,体外对PRD的耐药性与化疗的短期和长期临床反应显著相关,后者在PRD临床反应良好的亚组中也存在。儿童ALL中抗癌药物之间存在更普遍的体外交叉耐药性,尽管也认识到了药物的特异性活性。

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