Harasym T O, Cullis P R, Bally M B
British Columbia Cancer Agency, Vancouver, Canada.
Cancer Chemother Pharmacol. 1997;40(4):309-17. doi: 10.1007/s002800050662.
A pharmacological evaluation of an egg phosphatidylcholine/cholesterol (55:45 mole ratio, EPC/Chol) liposome doxorubicin formulation was carried out. The objective was to define liposomal lipid and drug distribution within sites of tumor growth following intravenous (i.v.) administration to female BDF1 mice bearing either Lewis lung carcinoma, B16/BL6 melanoma, or L1210 ascitic tumors.
Mice were injected i.v. with EPC/Chol liposomal doxorubicin, and plasma and tumor levels of lipid and drug were determined 1, 4 and 24 h late with radiolabeled lipid and fluorimetry or fluorescence microscopy, respectively. In addition, single-cell suspensions of the Lewis lung and B16/BL6 tumors were prepared and the presence of macrophages was determined with an FITC-labeled rat antimouse CD11b (MAC-1) antibody.
For mice bearing the Lewis lung solid tumors, there was a time-dependent accumulation of liposomal lipid, with a plateau of approximately 500 micrograms lipid/g tumor at 48 h. In contrast, the apparent plateau (microgram doxorubicin/g tumor) for doxorubicin was achieved at 1 h and remained constant over a 72-h time course. In comparison with free drug administered at the maximum tolerated dose (MTD, 20 mg/kg) doxorubicin levels in tumors were two- to threefold greater when the drug was administered in liposomal form. The increase in drug delivery was comparable for both solid tumors. With animals bearing the L1210 ascitic tumor, drug exposure was as much as ten times greater (in comparison with free drug) when doxorubicin was administered in liposomes. An evaluation of single-cell suspensions prepared from the two solid tumors suggested that more than 98% of the tumor-associated drug and liposomal lipid was not tumor cell-associated. Histological studies with the Lewis lung carcinoma, however, revealed that a proportion of the drug did colocalize with tumor-associated macrophages. Analysis of cells obtained from mice bearing ascitic tumors showed that more than 80% of the cell-associated drug could be removed by procedures designed to remove adherent cells.
The results summarized here suggest drug concentrations within a solid tumor, such as the Lewis lung carcinoma, are constant over time when the drug is given in a "leaky" EPC/Chol formulation. The results also suggest that liposomal lipid within sites of tumor growth is primarily localized within the interstitial spaces or tumor-associated macrophages.
对一种鸡蛋磷脂酰胆碱/胆固醇(摩尔比55:45,EPC/Chol)脂质体阿霉素制剂进行药理学评价。目的是确定静脉注射(i.v.)给患有Lewis肺癌、B16/BL6黑色素瘤或L1210腹水瘤的雌性BDF1小鼠后,脂质体脂质和药物在肿瘤生长部位的分布情况。
给小鼠静脉注射EPC/Chol脂质体阿霉素,分别在1、4和24小时后,用放射性标记脂质和荧光测定法或荧光显微镜法测定血浆和肿瘤中的脂质和药物水平。此外,制备Lewis肺癌和B16/BL6肿瘤的单细胞悬液,并用异硫氰酸荧光素(FITC)标记的大鼠抗小鼠CD11b(MAC-1)抗体测定巨噬细胞的存在情况。
对于患有Lewis肺癌实体瘤的小鼠,脂质体脂质存在时间依赖性积累,在48小时时达到约500微克脂质/克肿瘤的平台期。相比之下,阿霉素的表观平台期(微克阿霉素/克肿瘤)在1小时时达到,并在72小时的时间进程中保持恒定。与以最大耐受剂量(MTD,20毫克/千克)给予的游离药物相比,当以脂质体形式给药时,肿瘤中的阿霉素水平高出两到三倍。两种实体瘤的药物递送增加情况相当。对于患有L1210腹水瘤的动物,当阿霉素以脂质体形式给药时,药物暴露量(与游离药物相比)高出多达十倍。对从两种实体瘤制备的单细胞悬液的评估表明,超过98%的肿瘤相关药物和脂质体脂质与肿瘤细胞无关。然而,对Lewis肺癌的组织学研究表明,一部分药物确实与肿瘤相关巨噬细胞共定位。对患有腹水瘤的小鼠获得的细胞分析表明,超过80%的细胞相关药物可以通过旨在去除贴壁细胞的程序去除。
此处总结的结果表明,当以“渗漏性”EPC/Chol制剂给予药物时,实体瘤(如Lewis肺癌)内的药物浓度随时间保持恒定。结果还表明,肿瘤生长部位的脂质体脂质主要定位于间质间隙或肿瘤相关巨噬细胞内。
