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引用本文:陈莹,吴镁春,潘黎军,王驰.白介素-2靶向5-氟尿苷棕榈酸酯脂质体的制备及细胞毒性研究[J].中国现代应用药学,2011,28(9):842-845.
CHEN Ying,WU Meichun,PAN Lijun,WANG Chi.Preparation of 5′-Palmitoyl-5-Fluorouridine Liposomes Modified with Interleukin-2 and Its Cell Toxicity[J].Chin J Mod Appl Pharm(中国现代应用药学),2011,28(9):842-845.
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白介素-2靶向5-氟尿苷棕榈酸酯脂质体的制备及细胞毒性研究
陈莹, 吴镁春, 潘黎军, 王驰
重庆医科大学药学院,重庆 400016
摘要:
目的 制备了白介素-2(IL-2)靶向5-氟尿苷棕榈酸酯(5-FURP)脂质体,并进行了体外细胞毒性,初步考察其对IL-2受体高表达的肿瘤细胞的靶向作用。方法 采用逆相蒸发法制备5-FURP脂质体,通过交联剂将IL-2连接到脂质体的表面,得IL-2靶向5-FURP脂质体(IL-2-5FURP-L);UV法测定包封率;用考马斯亮蓝结合法测定IL-2与脂质体的结合率;用MTT法测定脂质体对IL-2受体高表达的皮肤T细胞淋巴瘤Hut-102细胞的生长抑制作用。结果 IL-2-5-FURP-L的粒径为180 nm;药物平均包封率为91.3%;IL-2的结合率为56.0%;在pH7.4的释放介质中,脂质体具有缓释作用;MTT实验结果显示,IL-2-5-FURP-L呈剂量依赖性抑制肿瘤细胞的生长,72 h细胞毒性试验表明IL-2-5-FURP-L对Hut-102的杀伤作用(IC50=1.04 μg·mL-1)明显优于5-FURP-L(IC50=6.11 μg·mL-1)及5-FURP(IC50=7.35 μg·mL-1)。结论 IL-2修饰的载药脂质体具有明显的抑瘤作用和主动靶向作用。
关键词:  白介素-2  5-氟尿苷棕榈酸酯  脂质体  主动靶向  细胞毒性实验
DOI:
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Preparation of 5′-Palmitoyl-5-Fluorouridine Liposomes Modified with Interleukin-2 and Its Cell Toxicity
CHEN Ying, WU Meichun, PAN Lijun, WANG Chi
College of Phamacy, Chongqing Medical University, Chongqing 400016, China
Abstract:
OBJECTIVE To investigate the specificity of interleukin-2 (IL-2) targeting liposomes (L) containing 5 ′ -palmitoyl- 5-fluorouridine (5-FURP). METHODS Liposomes containing 5-FURP were prepared by reverse phase evaporation method. IL-2 targeting 5-FURP-L were prepared through the effect of cross linker. The entrapment efficiency was measured by UV method. The amount of IL-2 conjugated to liposomes was determined with coomassie brilliant blue binding assay. Cytotoxicity on Hut-102 cells expressing IL-2 receptors in vitro was evaluated with MTT methods. RESULTS The mean size of the liposomes was 180 nm and the entrapment efficiency was 91.3%. The coupling efficiency of IL-2 was 56.0%. In pH 7.4 PBS , 5-FURP was released in a sustained manner from the liposomes. The MTT assay suggested that the IL-2 targeting 5-FURP-L had a distinct killing effect on Hut-102 tumor cells. CONCLUSION The IL-2 modified 5-FURP-L has an active targeting function and a significant anticancer effect.
Key words:  interleukin-2  5′-palmitoyl-5-fluorouridine  liposomes  active targeting  cell toxicity
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