Smart Nanocarrier Based on PEGylated Hyaluronic Acid for Cancer Therapy

纳米载体 细胞毒性 喜树碱 癌细胞 药理学 化学 体内分布 阿霉素 内吞作用 体内 透明质酸 癌症 毒品携带者 紫杉醇 癌症研究 体外 生物化学 药品 医学 受体 生物 化疗 内科学 生物技术 解剖
作者
Ki Young Choi,Hong Yeol Yoon,Jong‐Ho Kim,Sang Mun Bae,Rang‐Woon Park,Young Mo Kang,In-San Kim,Ick Chan Kwon,Kuiwon Choi,Seo Young Jeong,Kwangmeyung Kim,Jae Hyung Park
出处
期刊:ACS Nano [American Chemical Society]
卷期号:5 (11): 8591-8599 被引量:377
标识
DOI:10.1021/nn202070n
摘要

Tumor targetability and site-specific drug release of therapeutic nanoparticles are key factors for effective cancer therapy. In this study, poly(ethylene glycol) (PEG)-conjugated hyaluronic acid nanoparticles (P-HA-NPs) were investigated as carriers for anticancer drugs including doxorubicin and camptothecin (CPT). P-HA-NPs were internalized into cancer cells (SCC7 and MDA-MB-231) via receptor-mediated endocytosis, but were rarely taken up by normal fibroblasts (NIH-3T3). During in vitro drug release tests, P-HA-NPs rapidly released drugs when incubated with cancer cells, extracts of tumor tissues, or the enzyme Hyal-1, which is abundant in the intracellular compartments of cancer cells. CPT-loaded P-HA-NPs (CPT-P-HA-NPs) showed dose-dependent cytotoxicity to cancer cells (MDA-MB-231, SCC7, and HCT 116) and significantly lower cytotoxicity against normal fibroblasts (NIH-3T3) than free CPT. Unexpectedly, high concentrations of CPT-P-HA-NPs demonstrated greater cytotoxicity to cancer cells than free CPT. An in vivo biodistribution study indicated that P-HA-NPs selectively accumulated into tumor sites after systemic administration into tumor-bearing mice, primarily due to prolonged circulation in the blood and binding to a receptor (CD44) that was overexpressed on the cancer cells. In addition, when CPT-P-HA-NPs were systemically administrated into tumor-bearing mice, we saw no significant increases in tumor size for at least 35 days, implying high antitumor activity. Overall, P-HA-NPs showed promising potential as a drug carrier for cancer therapy.
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