Pharmacological studies of cisplatin encapsulated in long-circulating liposomes in mouse tumor models

被引:121
|
作者
Bandak, S [1 ]
Goren, D [1 ]
Horowitz, A [1 ]
Tzemach, D [1 ]
Gabizon, A [1 ]
机构
[1] Hebrew Univ Jerusalem, Hadassah Med Ctr, Sharet Inst Oncol, IL-91120 Jerusalem, Israel
关键词
cisplatin; liposomes; pharmacokinetics; SPI-077;
D O I
10.1097/00001813-199911000-00007
中图分类号
R73 [肿瘤学];
学科分类号
100214 ;
摘要
We investigated the pharmacokinetics and therapeutic efficacy of cisplatin encapsulated in polyethyleneglycol-coated long-circulating liposomes in a formulation referred to as SPI-077, in three mouse tumor models (M-109 lung carcinoma inoculated s.c,, J-6456 lymphoma inoculated i.p. and A-375 melanoma inoculated s.c.). Tumor-bearing mice were injected i.v. with single doses of SPI-077 and cisplatin, For pharmacokinetic experiments, mice were sacrificed at different timepoints post-treatment. Platinum levels were determined in plasma, spleen, liver, kidneys and tumors using flameless atomic absorption spectrophotometry, Survival times and/or tumor size were recorded for therapeutic studies. The pharmacokinetic studies revealed a prolonged circulation time and enhanced tumor uptake for SPI-077. In contrast to these results, no superior antitumor activity of SPI-077 over cisplatin could be observed in all tumor models, In vitro release experiments showed a negligible release (below 10%) of platinum from the liposomes, An in vitro cytotoxicity assay indicated a reduced cytotoxic activity of SPI-077 in comparison to cisplatin. We concluded that SPI-077 is being delivered to the tumor sites in a low bioavailability form, with extremely slow release kinetics. This explains the discrepant results of high platinum concentrations in tumors and reduced therapeutic activity after administration of SPI-077. [(C) 1999 Lippincott Williams & Wilkins.].
引用
收藏
页码:911 / 920
页数:10
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