Hida T, Ueda R, Takahashi T, Watanabe H, Kato T, Suyama M, Sugiura T, Ariyoshi Y, Takahashi T
Laboratory of Chemotherapy, Aichi Cancer Center, Nagoya, Japan.
Cancer Res. 1989 Sep 1;49(17):4785-90.
The 3-(4,5-Dimethylthiazol-2-yl)-2,5-diphenyltetrazolium bromide (MTT) hybrid assay was developed by technically combining the human tumor clonogenic assay and the MTT assay to make the most of both assays. This assay was able to estimate the in vitro growth of cultured cell lines and of tumor cells in pleural effusion, suggesting the possibility of its use for assessment of chemosensitivity and radiosensitivity of fresh tumor samples. Multiple cell lines [including morphological and/or phenotypical in vitro converters and cisplatin (CDDP)-resistant lines] were established from three patients with small cell lung cancer at different stages of the disease. Chemosensitivity of these cell lines to four commonly used chemotherapeutic drugs was tested by the MTT hybrid assay. SK1 and SK3 lines were established from Patient S. K. before and after chemotherapy and radiotherapy, respectively. SK3/CDDP, a CDDP-resistant line derived from the SK3 line, was 30-fold more resistant to CDDP [50% inhibiting dose (IC50), 21.5 micrograms/ml] than the SK1 line. In Patient M. O., MOA2/CDDP, a CDDP-resistant line derived from MOA2 (an in vitro converter from the MO line), was 41-fold more resistant to CDDP (IC50, 37 micrograms/ml) than the parent MO line. From Patient T. M., TM1 and TM2 lines were established before and after chemotherapy, respectively. The latter showed 6-fold more resistance to CDDP than the former. Chemosensitivity of these lines to three other drugs, 4-hydroperoxycyclophosphamide, Adriamycin, and etoposide, suggested cross-resistance between CDDP and 4-hydroperoxycyclophosphamide. Radiosensitivity study was also carried out with the MTT hybrid assay. The MOA2 line was more resistant [Do, 3.0 Gy; extrapolation number (n), 4.0] than the parental MO line (Do, 1.6 Gy; n, 2.1). There was no clear difference in radiosensitivity between the cell lines established before and after radiation therapy in Patient S. K.
通过技术上结合人肿瘤克隆形成试验和MTT试验开发了3-(4,5-二甲基噻唑-2-基)-2,5-二苯基四氮唑溴盐(MTT)杂交试验,以充分利用这两种试验。该试验能够评估培养细胞系以及胸腔积液中肿瘤细胞的体外生长情况,提示其可用于评估新鲜肿瘤样本的化学敏感性和放射敏感性。从三名处于疾病不同阶段的小细胞肺癌患者中建立了多个细胞系[包括形态学和/或表型体外转化细胞系和顺铂(CDDP)耐药细胞系]。通过MTT杂交试验检测了这些细胞系对四种常用化疗药物的化学敏感性。SK1和SK3细胞系分别从患者S.K.化疗和放疗前、后建立。SK3/CDDP是从SK3细胞系衍生而来的CDDP耐药细胞系,对CDDP[50%抑制剂量(IC50),21.5微克/毫升]的耐药性比SK1细胞系高30倍。在患者M.O.中,MOA2/CDDP是从MOA2(MO细胞系的体外转化细胞系)衍生而来的CDDP耐药细胞系,对CDDP(IC50,37微克/毫升)的耐药性比亲代MO细胞系高41倍。从患者T.M.中,分别在化疗前和化疗后建立了TM1和TM2细胞系。后者对CDDP的耐药性比前者高6倍。这些细胞系对其他三种药物4-氢过氧环磷酰胺、阿霉素和依托泊苷的化学敏感性提示CDDP和4-氢过氧环磷酰胺之间存在交叉耐药性。还用MTT杂交试验进行了放射敏感性研究。MOA2细胞系比亲代MO细胞系更耐药[Do,3.0 Gy;外推数(n),4.0](Do,1.6 Gy;n,2.1)。患者S.K.放疗前和放疗后建立的细胞系之间在放射敏感性方面没有明显差异。
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