Hyaluronic acid-coated silver nanoparticles releasing Doxorubicin for combinatorial antitumor therapy

被引:0
|
作者
Thi, Phuong Le [1 ,2 ]
Nguyen, Dinh Trung [3 ,4 ]
Huu, Thien An Nguyen [2 ]
Tran, Quang-Hieu [5 ]
Truong, Minh-Dung [6 ]
Hang, Ngo Thanh [7 ]
Tran, Ngoc Quyen [1 ,2 ]
Park, Ki Dong [8 ]
机构
[1] Vietnam Acad Sci & Technol, Inst Appl Mat Sci, Ho Chi Minh City 700000, Vietnam
[2] Vietnam Acad Sci & Technol, Grad Univ Sci & Technol, Ho Chi Minh City 700000, Vietnam
[3] Duy Tan Univ, Inst Fundamental & Appl Sci, Ho Chi Minh City 700000, Vietnam
[4] Duy Tan Univ, Fac Nat Sci, Da Nang 550000, Vietnam
[5] Saigon Technol Univ, Basic Sci Dept, 180 Cao Lo,Ward 4,Dist 8, Ho Chi Minh City 700000, Vietnam
[6] Biotechnol Ctr Ho Chi Minh City, Ho Chi Minh City 700000, Vietnam
[7] Ajou Univ, Mol Sci & Technol Res Ctr MSTRC, Suwon 16499, South Korea
[8] Ajou Univ, Dept Mol Sci & Technol, Suwon 16499, South Korea
关键词
Nanoparticle; Hyaluronic acid; Targeting delivery; Synergistic anti-cancer therapy; STIMULI-RESPONSIVE NANOCARRIERS; TUMOR MICROENVIRONMENT; DRUG-DELIVERY; CANCER; GENERATION; OXIDE;
D O I
10.1016/j.jiec.2024.07.049
中图分类号
O6 [化学];
学科分类号
0703 ;
摘要
Although various nanocarriers have been developed to deliver anticancer drugs to the target tumors, it is still remaining great challenges, including burst release, non-specific targetability and insufficient therapeutic efficacy. Herein, we prepared a multifunctional nanoparticle composed of Ag core and hyaluronic acid shell (Ag NPs@HA) for stimultaneously intracellular delivery of Doxorubicin (DOX) and Ag NPs to improve the anticancer therapeutic efficacy. For our approach, Ag NPs was simply synthesized via the redox reaction between Ag+ ions and catechol group of functional HA, and DOX was subsequently loaded into the HA-coated Ag NPs through the interaction between the remaining catechol groups and DOX (Ag NPs@HA/DOX). The particles exhibited uniform morphology, good biocompatibility to normal cells, and pH-sensitive drug release. Notably, thanks to the specific interaction of HA and CD44 receptor-overexpressing cancer cells, Ag NPs@HA/DOX could dramatically improve the anti-tumor efficacy in vitro as well as in vivo mimicking 3D spheroid model, compared to the free DOX. Moreover, Ag NPs@HA/DOX exhibited superior tumor supression in vivo on a HELA-xenografted mouse model, while minimizing the systemic toxicity of free DOX. From the obtained results, we suggest Ag NPs@HA as potential nanocarrier for targeting delivery of various therapeutic drugs in anticancer therapy.
引用
收藏
页码:431 / 440
页数:10
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