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氨柔比星对其活性代谢物的体内疗效及肿瘤选择性代谢

In vivo efficacy and tumor-selective metabolism of amrubicin to its active metabolite.

作者信息

Noguchi T, Ichii S, Morisada S, Yamaoka T, Yanagi Y

机构信息

Research Center, Sumitomo Pharmaceuticals Co., Ltd., Osaka.

出版信息

Jpn J Cancer Res. 1998 Oct;89(10):1055-60. doi: 10.1111/j.1349-7006.1998.tb00496.x.

Abstract

The tissue distribution of a novel antitumor anthracycline antibiotic, amrubicin, was studied using seven human tumor xenografts implanted into nude mice, in order to identify the principal factors determining its therapeutic efficacy. We found a good correlation between the level of the metabolite amrubicinol in the tumor and the in vivo efficacy. High metabolic activity of amrubicin to amrubicinol was detected in tumor tissue homogenates, especially in cell lines highly sensitive to amrubicin in vivo. In contrast to amrubicin, the administration of amrubicinol showed less tumor-selective toxicity in these human tumor xenograft models. These data indicate that the tumor-selective metabolism of amrubicin to amrubicinol resulted in a tumor-selective disposition of amrubicinol, leading to good efficacy in in vivo experimental therapeutic models.

摘要

为了确定决定新型抗肿瘤蒽环类抗生素氨柔比星治疗效果的主要因素,我们使用植入裸鼠体内的七种人类肿瘤异种移植模型研究了其组织分布。我们发现肿瘤中代谢产物氨柔比星醇的水平与体内疗效之间存在良好的相关性。在肿瘤组织匀浆中检测到氨柔比对氨柔比星醇的高代谢活性,尤其是在体内对氨柔比星高度敏感的细胞系中。与氨柔比星不同,在这些人类肿瘤异种移植模型中,氨柔比星醇的给药显示出较低的肿瘤选择性毒性。这些数据表明,氨柔比星向氨柔比星醇的肿瘤选择性代谢导致了氨柔比星醇的肿瘤选择性分布,从而在体内实验治疗模型中产生了良好的疗效。

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