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乏氧细胞增敏剂米索硝唑在人肿瘤克隆试验中对集落形成的直接作用

Direct effects of the hypoxic cell sensitizer misonidazole on colony formation in a human tumor cloning assay.

作者信息

Scheithauer W, Von Hoff D D, Forseth B, Cowan J D

出版信息

Cancer Drug Deliv. 1986 Winter;3(1):15-24. doi: 10.1089/cdd.1986.3.15.

Abstract

The human tumor cloning assay as described by Hamburger and Salmon was utilized to study the direct antitumor effects of the hypoxic cell sensitizer misonidazole (MISO). Cells from 106 tumor specimens directly obtained from patients were exposed to MISO at clinically achievable drug concentrations (0.5 mM). Of 30 evaluable tumors, seven specimens (23%) showed a less than or equal to 50% decrease of TCFU's. In vitro sensitivity to MISO was noted in human breast cancer, renal cancer, non small-cell lung cancer, and adenocarcinoma of unknown primary site. A dose response relationship was demonstrated in a subset of experiments including 6 patient's tumors and one human breast cancer cell-line. An analysis relating MISO sensitivity or resistance to the results obtained with other, simultaneously tested standard anticancer drugs indicated that tumors exhibiting a less than or equal to 50% decrease of TCFU's in the presence of MISO were also likely to be sensitive to other cytotoxic drugs. In summary, our data suggest that the 'nitroimidazoles' may exert clinically significant direct antitumor effects in individual tumors. The human tumor cloning assay may have potential to evaluate these direct effects of MISO-analogues and other new radiosensitizers currently being tested in clinical trials.

摘要

采用汉堡和萨蒙所描述的人肿瘤克隆试验,研究乏氧细胞增敏剂米索硝唑(MISO)的直接抗肿瘤作用。从106例直接取自患者的肿瘤标本中获取的细胞,在临床可达到的药物浓度(0.5 mM)下暴露于米索硝唑。在30个可评估的肿瘤中,7个标本(23%)显示肿瘤克隆形成单位(TCFU)减少小于或等于50%。在人乳腺癌、肾癌、非小细胞肺癌和原发部位不明的腺癌中观察到对米索硝唑的体外敏感性。在包括6例患者肿瘤和1个人乳腺癌细胞系的一组实验中证明了剂量反应关系。将米索硝唑敏感性或耐药性与同时检测的其他标准抗癌药物的结果进行分析表明,在米索硝唑存在下TCFU减少小于或等于50%的肿瘤也可能对其他细胞毒性药物敏感。总之,我们的数据表明“硝基咪唑类”可能在个体肿瘤中发挥具有临床意义的直接抗肿瘤作用。人肿瘤克隆试验可能有潜力评估米索硝唑类似物和目前正在临床试验中测试的其他新型放射增敏剂的这些直接作用。

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