卡培他滨乳腺组织穿透及向氟脲嘧啶转化的药动学研究

卡培他滨乳腺组织穿透及向氟脲嘧啶转化的药动学研究

叶敏^*, 朱珠, 付强, 孙强, 茅枫

1.中国医学科学院中国协和医科大学北京协和医院药剂科, 北京 100730;
2.中国医学科学院中国协和医科大学北京协和医院乳腺外科, 北京 100730

收稿日期:2006-03-12 修回日期:2006-08-10 出版日期:2006-09-15 发布日期:2006-09-15
通讯作者: 叶敏*

Tissue Penetration of Capecitabine and Its Tumor-Selective Delivery of 5-FU in Advanced Breast Cancer Patients

YE Min^*, ZHU Zhu, FU Qiang, SUN Qiang, MAO Feng

1.Department of Pharmacy, Peking Union Medical College Hospital, Academy of Chinese Medical Sciences, Beijing 100730, China;
2.Department of Surgery, Peking Union Medical College Hospital, Academy of Chinese Medical Sciences, Beijing 100730, China

Received:2006-03-12 Revised:2006-08-10 Online:2006-09-15 Published:2006-09-15
Contact: YE Min*

摘要/Abstract

摘要： 目的描述卡培他滨在血浆、乳腺肿瘤组织和正常组织中向氟脲嘧啶转化的药物动力学过程。方法 27名乳腺癌化疗患者口服卡培他滨1255 mg·m^-2, 同步采集血浆、肿瘤组织和相邻正常组织样品, 并用HPLC法测定卡培他滨和5-FU的浓度。使用自建的药物动力学模型拟合卡培他滨和5-FU的药时曲线, 并利用拟合参数计算血浆和乳腺组织中卡培他滨和5-FU的组织分布因子, 以及卡培他滨向5-FU的转化率。结果卡培他滨在肿瘤组织中的组织分布因子(AUC_Tumor/AUC_plasma)为0.6371, 正常组织中的组织分布因子(AUC_H-tissue/AUC_plasma)为0.8514; 5-FU在乳腺肿瘤的组织分布因子AUC_Tumor/AUC_plasma为3.9926, 正常组织的组织分布因子AUC_H-tissue/AUC_plasma为2.4380。卡培他滨向5-FU的转化率在肿瘤、邻近正常组织和血浆中分别为1.026、0.4895和0.163。结论血浆、乳腺肿瘤组织和相邻正常组织的药时曲线拟合对卡培他滨转化为5-FU及5-FU消除过程进行了较好的描述。卡培他滨在血浆、乳腺肿瘤组织和相邻正常组织中的分布较为接近, 其活性代谢产物5-FU在肿瘤组织中分布为血浆的10.14倍, 为正常组织的3.41倍。卡培他滨在肿瘤组织中向5-FU的转化率较高。

关键词: 卡培他滨, 卡培他滨, 卡培他滨, 药物动力学, 药物动力学, 药物动力学, 氟脲嘧啶, 氟脲嘧啶, 氟脲嘧啶, 组织分布因子, 组织分布因子, 组织分布因子

Abstract: Aim To measure the penetration of capecitabine from the plasma into tissue and to investigate the pharmacokinetics of its metabolizing into fluorouracil (5-FU) in patients with advanced breast cancer. Methods Twenty-seven patients with breast cancer received repeated doses of 1255 mg·m^-2 of capecitabine twice daily for 7 d. Blood, tumor, and adjacent healthy tissue samples were collected. The concentrations of capecitabine and its metabolite 5-FU were determined by HPLC. The concentration-time profiles of capecitabine and 5-FU were fitted by pharmacokinetic model. The tissue distribution factors for capecitabine and 5-FU, and the AUC ratios of 5-FU to capecitabine in plasma, tumor or adjacent healthy tissue, were calculated with pharmacokinetic parameters, respectively. Results The Ka of capecitabine was 1.17 h^-1 in plasma, 0.46 h^-1 in tumor tissue, and 0.61 h^-1 in healthy tissue. The AUCs of capecitabine were 2.5571 μg·mL^-1·h, 1.6292 μg·g^-1·h and 2.0850 μg·g^-1·h, and T_1/2 was 0.7823 h, 1.5281 h and 1.2896 h in plasma, tumor, and healthy tissue, respectively. The AUCs of 5-FU were 0.4187 μg·mL^-1·h, 1.6717 μg·g^-1 ·h and 1.0208 μg·g^-1 ·h; the T_1/2 was 0.6313 h , 1.2041 h and 1.0312 h in plasma, tumor, and healthy tissue, respectively. The tissue distribution factors of capecitabine were 0.6371 in tumor (AUC_cap-Tumor/AUC_cap-plasma) and 0.8514 in healthy tissue (AUC_cap-HT/AUC_cap-plasma). The tissue distribution factors of 5-FU were 3.992 6 in tumor (AUC_5-FU-tumor/AUC_5-FU-plasma) and 2.4380 in healthy tissue (AUC_5-FU-HT/AUC_5-FU-plasma). The AUC ratios of 5-FU to capecitabine were 0.1637, 1.0261, and 0.4895 in plasma, tumor, and healthy tissue, respectively. Conclusion The simulation curves for the disposition of capecitabine and its metabolite 5-FU in plasma and tissue basically describe the activation process of capecitabine metabolizing to 5-FU and 5-FU elimination. There are similar distributions for capecitabine in plasma, tumor, and healthy tissue. The exposure of 5-FU in tumor was found to be 3.992 6 times greater than that in plasma and 2.438 0 times greater than that in healthy tissue. Capecitabine may metabolize preferentially to 5-FU in tumor tissue after oral administration.

Key words: capecitabine, capecitabine, pharmacokinetics, pharmacokinetics, 5-FU, 5-FU, tissue distribution factors, tissue distribution factors

中图分类号:

R969.1

Supporting: ^*Corresponding author. Tel.: 86-10-65296537

叶敏^*, 朱珠, 付强, 孙强, 茅枫. 卡培他滨乳腺组织穿透及向氟脲嘧啶转化的药动学研究[J]. .

YE Min^*, ZHU Zhu, FU Qiang, SUN Qiang, MAO Feng. Tissue Penetration of Capecitabine and Its Tumor-Selective Delivery of 5-FU in Advanced Breast Cancer Patients[J]. .

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