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Tumor site-specific PEG detachment and active tumor homing of therapeutic PEGylated chitosan/folate-decorated polydopamine nanoparticles to augment antitumor efficacy of photothermal/chemo combination therapy

光热治疗 化学 纳米颗粒 乙二醇 PEG比率 体内 叶酸受体 药物输送 壳聚糖 阿霉素 生物物理学 纳米技术 材料科学 癌细胞 生物化学 癌症 化疗 有机化学 医学 生物技术 经济 外科 内科学 生物 财务
作者
Ming-Hung Hsieh,Tzu-Hao Wang,Shang-Hsiu Hu,Tsai-Ching Hsu,Jia-Le Yow,Bor-Show Tzang,Wen-Hsuan Chiang
出处
期刊:Chemical Engineering Journal [Elsevier]
卷期号:446: 137243-137243 被引量:14
标识
DOI:10.1016/j.cej.2022.137243
摘要

• Co-deposition of BI-PC adducts and DA molecules formed core–shell nanoparticles. • Hybrid nanoparticles showed prominent acid and photothermal-triggered DOX release. • Cellular uptake of hybrid nanoparticles was promoted by dePEGylation and FA exposure. • Hybrid nanoparticles largely inhibited tumor growth by photothermal/chemo therapy. To effectively promote tumor-targeted delivery of photothermal/chemo combined therapy for boosted antitumor efficacy, the versatile photothermal hybrid polymeric nanoparticles capable of detaching poly(ethylene glycol) (PEG) segments and exposing tumor-targeting folate (FA) moieties in response to tumor extracellular acidity (pH e ) are developed to selectively deliver doxorubicin (DOX), a chemotherapy drug, to the tumor sites. Through one-pot co-deposition of dopamine molecules with acidity-responsive benzoic imine-containing PEGylated chitosan (BI-PC) adducts, the hybrid BI-PC/polydopamine (PDA) nanoparticles were attained as DOX vehicles and characterized to have a spherical structure composed of a PDA core surrounded by hydrophilic BI-PC shells. The DOX@BI-PC/PDA nanoparticles not only showed prominent colloidal stability in serum-containing environment and photothermal conversion efficiency, but also exhibited acidity/photothermal-activated drug release. The PEG detachment and FA exposure of FA-DOX@BI-PC/PDA nanoparticles in weak acidic environment appreciably promoted their uptake by FA receptor-overexpressed CT-26 colon cancer cells, thus largely augmenting anticancer potency based on the photothermal/chemo therapy. Importantly, the pH e -responsive FA-DOX@BI-PC/PDA nanoparticles markedly accumulated in CT-26 tumor sites in vivo and inhibited tumor growth without significant systemic toxicity upon the near infrared (NIR)-triggered hyperthermia integrated with DOX chemotherapy. This work presents a practical strategy for improved antitumor potency of photothermal/chemo combination therapy.
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