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CONVERSION OF MITOMYCIN-C TO 2,7-DIAMINOMITOSENE AND 10-DECARBAMOYL 2,7-DIAMINOMITOSENE IN TUMOR-TISSUE IN-VIVO

被引:1
作者
CHIRREY, L
CUMMINGS, J
HALBERT, GW
SMYTH, JF
机构
[1] WESTERN GEN HOSP,IMPERIAL CANC RES FUND,MED ONCOL UNIT,EDINBURGH EH4 2XU,MIDLOTHIAN,SCOTLAND
[2] UNIV STRATHCLYDE,DEPT PHARM,GLASGOW G1 1XW,LANARK,SCOTLAND
来源
CANCER CHEMOTHERAPY AND PHARMACOLOGY | 1995年 / 35卷 / 04期
关键词
MITOMYCIN C; IN VIVO; TUMOR; METABOLISM;
D O I
10.1007/s002800050239
中图分类号
R73 [肿瘤学];
学科分类号
100214 ;
摘要
The progress of mitomycin C (MMC) bioreduction was studied in vivo in the rat Sp 107 mammary carcinoma after intra-tumoural injection of either 100 mu g or 1 mg. 2,7-Diaminomitosene (2,7-DM) was utilised as a primary bioreductive metabolite and 10-decarbamoyl 2,7-diaminomitosene (DC 2,7-DM) served as a secondary bioreductive metabolite, both of which were measured by high-performance liquid chromatography. 2,7-DM and DC 2,7-DM were produced rapidly, achieving close to their maximal concentrations at the earliest time point studied [5 min]. 2,7-DM was cleared rapidly from the tumour with apparent half-lives of 5 and 35 min after the low and high drug doses, respectively. DC 2,7-DM had a longer apparent half-life of 130 min at the higher dose but, as compared with 2,7-DM, was only a minor metabolite [the area under the curve (AUC) of 2,7-DM was 5.6-fold that of DC 2,7-DM]. At the lower drug dose, DC 2,7-DM was not detectable. Rapid formation and disappearance of bioreductive metabolites of MMC may account for the failure of previous studies to detect these products in vivo.
引用
收藏
页码:318 / 322
页数:5
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