载紫杉醇的PEG修饰的大黄酸偶联物胶束的细胞摄取及活体成像研究

李崇仙; 王夏英; 陆伟利; 郑雅玲; 许雪雅; 王晓颖<sup>*</sup>; 徐伟<sup>*</sup>

引用本文:	李崇仙,王夏英,陆伟利,郑雅玲,许雪雅,王晓颖,徐伟.载紫杉醇的PEG修饰的大黄酸偶联物胶束的细胞摄取及活体成像研究[J].中国现代应用药学,2023,40(13):1753-1758.
	LI Chongxian,WANG Xiaying,LU Weili,ZHENG Yaling,XU Xueya,WANG Xiaoying,XU Wei.Study on Cellular Uptake and in Vivo Imaging of Paclitaxel-loaded PEG-modified Rhein Conjugate Micelles[J].Chin J Mod Appl Pharm(中国现代应用药学),2023,40(13):1753-1758.

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载紫杉醇的PEG修饰的大黄酸偶联物胶束的细胞摄取及活体成像研究
李崇仙, 王夏英, 陆伟利, 郑雅玲, 许雪雅, 王晓颖, 徐伟
福建中医药大学, 福州 350122

摘要:

目的探究载紫杉醇(paclitaxel,PTX)的聚乙二醇(polyethylene glycol,PEG)修饰的大黄酸偶联物胶束的细胞摄取及活体成像情况。方法将环境响应型荧光探针P4/P2与药物PTX共载于mPEG-羧甲基壳聚糖-大黄酸(CRmP)偶联物胶束中,制备(P4+PTX)/CRmP胶束。以MCF-7细胞为细胞模型,利用激光共聚焦显微镜和流式细胞仪分析该胶束被MCF-7细胞摄取的情况;以H22皮下移植瘤小鼠为模型,在体和离体成像分析该胶束在体内的分布情况。结果 (P4+PTX)/CRmP胶束以完整的胶束形式被MCF-7细胞内吞摄入,分布于细胞质。(P2+PTX)/CRmP胶束在荷瘤小鼠的肝脏和肿瘤部位较多聚集,并于实验时间内在肿瘤部位不断累积。结论该胶束以完整的胶束形式被肿瘤细胞摄取,在体内有一定的肝靶向性和肿瘤靶向性。

关键词: 紫杉醇 PEG修饰的羧甲基壳聚糖-大黄酸偶联物聚合物胶束细胞摄取活体成像

DOI：10.13748/j.cnki.issn1007-7693.20223352

分类号:R965.2

基金项目:国家自然科学基金项目(81603301)；福建省科技厅引导性项目(2020Y0050)

Study on Cellular Uptake and in Vivo Imaging of Paclitaxel-loaded PEG-modified Rhein Conjugate Micelles

LI Chongxian, WANG Xiaying, LU Weili, ZHENG Yaling, XU Xueya, WANG Xiaoying, XU Wei

Fujian University of Traditional Chinese Medicine, Fuzhou 350122, China

Abstract:

OBJECTIVE To investigate the cellular uptake and in vivo imaging of paclitaxel(PTX)-loaded polyethylene glycol(PEG)-modified rhein conjugate micelles. METHODS (P4/P2+PTX)/CRmP micelles were prepared by co-loading environment-responsive fluorescent probes P4/P2 and PTX into CRmP micelles. Using MCF-7 cells as cell models, the uptake of the micelles by MCF-7 cells was analyzed by laser confocal microscopy and flow cytometry. The H22 subcutaneous transplanted tumor mice were used as animal models, and the distribution of the micelles in vivo and in vitro were analyzed by in vivo imaging system. RESULTS (P4+PTX)/CRmP micelles in the intact form were internalized by MCF-7 cells and distributed in the cytoplasm. (P2+PTX)/CRmP micelles were more accumulated in the liver and tumor sites in vivo, and gradually accumulated at the tumor sites during the experimental time. CONCLUSION The intact micelles can be taken up by tumor cells, and have liver and tumor targeting properties in vivo.

Key words: paclitaxel PEG-modified carboxymethyl chitosan-rhein conjugate polymer micelles cellular uptake in vivo imaging