Smart nanoparticles assembled by endogenous molecules for siRNA delivery and cancer therapy via CD44 and EGFR dual-targeting

被引:25
|
作者
Liang, Yaoyao [1 ]
Peng, Jiahui [1 ]
Li, Ning [2 ]
Yu-Wai-Man, Cynthia [3 ,4 ]
Wang, Qian [1 ]
Xu, Yuhong [1 ]
Wang, Hongxia [2 ]
Tagalakis, Aristides D. [5 ]
Du, Zixiu [1 ]
机构
[1] Shanghai Jiao Tong Univ, Sch Pharm, Shanghai, Peoples R China
[2] Shanghai Jiao Tong Univ, Sch Med, Shanghai Gen Hosp, Dept Oncol, Shanghai, Peoples R China
[3] Moorfields Eye Hosp NHS Fdn Trust, Natl Inst Hlth Res NIHR Biomed Res Ctr, London, England
[4] UCL Inst Ophthalmol, London, England
[5] Edge Hill Univ, Dept Biol, Ormskirk, England
基金
中国国家自然科学基金;
关键词
Dual targeting; CD44 and EGFR; Multifunctional peptide; Tumor; HA coating; PEPTIDE; NANOCOMPLEXES; DNA; EFFICIENT; RECEPTOR; GROWTH; DRUG;
D O I
10.1016/j.nano.2018.09.018
中图分类号
TB3 [工程材料学];
学科分类号
0805 ; 080502 ;
摘要
We developed an anticancer siRNA delivery system (named HLPR) through modular assembly of endogenous molecules. The structure of HLPR was a tightly condensed siRNA-peptide inner core in turn surrounded by the disordered lipid layer and thin HA coating from which the EGFR-targeted amino acid sequences of YHWYGYTPQNVI partially protrude outside of cell surfaces. Both HA and YHWYGYTPQNVI anchored on HLPR were responsible for targeting CD44 and EGFR overexpressed on the tumor cell surfaces, respectively. HLPR was relatively stable in the blood circulation and reached the tumor tissue in vivo through passive and active targeting. Then HLPR entered tumor cells mainly through EGFR-mediated pathway followed by the separation of HA from the remaining parts of nanocomplexes. The HA-uncoated complexes escaped the endosome through the membrane fusion function of DOPE and released cargoes (siRNAand peptide/siRNA) in the cytoplasm. HLPR significantly inhibited the growth of implanted subcutaneous liver tumors without toxicity. (C) 2018 Elsevier Inc. All rights reserved.
引用
收藏
页码:208 / 217
页数:10
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