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通过MTT法评估抗肿瘤药物:抗增殖特性的部分低估。

Assessment of antineoplastic agents by MTT assay: partial underestimation of antiproliferative properties.

作者信息

Sobottka S B, Berger M R

机构信息

Institute of Toxicology and Chemotherapy, German Cancer Research Center, Heidelberg.

出版信息

Cancer Chemother Pharmacol. 1992;30(5):385-93. doi: 10.1007/BF00689967.

DOI:10.1007/BF00689967
PMID:1505077
Abstract

In the present study a slightly modified MTT assay was used in conjunction with cell counting to determine the antiproliferative efficacy of N-(2-chloroethyl)-N-nitroso-N'-2-hydroxyethylurea (HECNU), vinblastine, and hexadecylphosphocholine (HPC) in a panel of six tumor cell lines. This panel consisted of two human (MDA-MB231, MCF-7) and two rodents (1/C2, 1/C32) mammary-carcinoma cell lines as well as of two tumor cell lines of gastrointestinal origin (HT-29, KB). It was shown that the use of acid isopropanol as a solvent of the formazan crystals produced correlations between cell number and absorption that were as good as, if not better than, those seen after dimethylsulfoxide (DMSO) application. The optimal period of incubation with the MTT dye was 2 h. A comparison of the antiproliferative activity of HECNU revealed that the HT-29 cell line was most resistant [50% inhibition concentration (IC50), 138.7 mumol/l], followed by MCF-7 cells (IC50, 127.7 mumol/l), whereas MDA-MB231 cells showed the highest sensitivity (IC50, 6 mumol/l). Vinblastine induced the highest (MCF-7 cells; IC50, 0.68 nmol/l) and the lowest (1/C2 cells; IC50, 7.69 nmol/l) degrees of growth inhibition in cell lines derived from mammary carcinoma. This contrasted with the activity of HPC, which was considerably less effective in the four mammary-carcinoma cell lines (IC50 from 29.4 to 69.9 mumol/l) than in the two cell lines of gastrointestinal origin (IC50, 1.9 and 3.1 mumol/l). Interestingly, treatment with HPC stimulated the growth of 1/C32 cells in the lower dose range. After treatment with HECNU, the average IC50 value determined in the MTT assay was 2.4-fold that disclosed by cell counting, whereas the average values found for HPC and vinblastine by both methods corresponded fairly well, with the respective values obtained using the MTT assay being only 26% and 14% higher than those measured by cell counting. A dose-dependent increase in the mean size of MCF-7 cells was observed after exposure to HECNU, which--if taken into account--considerably reduced underestimation of this parameter by the MTT assay. No variation in cell size was noted following treatment with HPC and vinblastine. Thus, depending on the antitumor agent used, the MTT assay can result in slight or even considerable underestimation of the antitumor efficacy of certain compounds and may need correction by consideration of the effect of the drugs on cell size.

摘要

在本研究中,我们使用了一种略作修改的MTT法,并结合细胞计数来测定N-(2-氯乙基)-N-亚硝基-N'-2-羟乙基脲(HECNU)、长春碱和十六烷基磷胆碱(HPC)对一组六种肿瘤细胞系的抗增殖效果。该细胞系包括两种人类(MDA-MB231、MCF-7)和两种啮齿动物(1/C2、1/C32)乳腺癌细胞系,以及两种胃肠道来源的肿瘤细胞系(HT-29、KB)。结果表明,使用酸性异丙醇作为甲臜晶体的溶剂,细胞数量与吸光度之间的相关性与使用二甲基亚砜(DMSO)时相当,甚至更好。MTT染料的最佳孵育时间为2小时。对HECNU抗增殖活性的比较显示,HT-29细胞系最耐药[50%抑制浓度(IC50),138.7 μmol/L],其次是MCF-7细胞(IC50,127.7 μmol/L),而MDA-MB231细胞表现出最高的敏感性(IC50,6 μmol/L)。长春碱在源自乳腺癌的细胞系中诱导的生长抑制程度最高(MCF-7细胞;IC50,0.68 nmol/L),最低(1/C2细胞;IC50,7.69 nmol/L)。这与HPC的活性形成对比,HPC在四种乳腺癌细胞系中的效果(IC50为29.4至69.9 μmol/L)远不如在两种胃肠道来源的细胞系中(IC50,1.9和3.1 μmol/L)。有趣的是,在较低剂量范围内,用HPC处理刺激了1/C32细胞的生长。用HECNU处理后,MTT法测定的平均IC50值是细胞计数法所揭示值的2.4倍,而HPC和长春碱通过两种方法得到的平均值相当吻合,MTT法得到的各自值仅比细胞计数法测量的值高26%和14%。在暴露于HECNU后,观察到MCF-7细胞的平均大小呈剂量依赖性增加,这一点如果考虑在内,会大大减少MTT法对该参数的低估。用HPC和长春碱处理后未观察到细胞大小的变化。因此,根据所使用的抗肿瘤药物不同,MTT法可能会导致对某些化合物的抗肿瘤效果略有低估甚至大幅低估,可能需要通过考虑药物对细胞大小的影响进行校正。

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