Nanovesicle-mediated systemic delivery of microRNA-34a for CD44 overexpressing gastric cancer stem cell therapy

被引:66
|
作者
Jang, Eunji [1 ,2 ]
Kim, Eunjung [1 ,3 ,4 ]
Son, Hye-Young [2 ,5 ]
Lim, Eun-Kyung [6 ,10 ]
Lee, Hwunjae [2 ,7 ]
Choi, Yuna [2 ,5 ]
Park, Kwangyeol [2 ,5 ]
Han, Seungmin [1 ]
Suh, Jin-Suck [2 ,5 ,8 ,9 ]
Huh, Yong-Min [2 ,5 ,8 ,9 ]
Haam, Seungjoo [1 ]
机构
[1] Yonsei Univ, Dept Chem & Biomol Engn, Coll Engn, Seoul 120749, South Korea
[2] SBSI, Seoul 120752, South Korea
[3] Imperial Coll London, Dept Bioengn, Dept Mat, London SW7 2AZ, England
[4] Imperial Coll London, Inst Biomed Engn, London SW7 2AZ, England
[5] Yonsei Univ, Dept Radiol, Coll Med, Seoul 120752, South Korea
[6] Korea Res Inst Biosci & Biotechnol, Hazards Monitoring Bionano Res Ctr, Daejeon 34141, South Korea
[7] Yonsei Univ, Nanomed Interdisciplinary Program, Natl Core Res Ctr, Seoul 120749, South Korea
[8] YUHS KRIBB Med Convergence Res Inst, Seoul 120752, South Korea
[9] Yonsei Univ, Coll Med, Brain Korea Project Med Sci 21, Seoul 120752, South Korea
[10] Univ Sci & Technol, Major Nanobiotechnol & Bioinformat, Daejeon 34113, South Korea
基金
新加坡国家研究基金会;
关键词
miR-34a delivery; CD44; suppression; Cancer stem cells; Nanovesicles; pH-responsive; PROSTATE-CANCER; BREAST-CANCER; MIR-34A; DRUG; MARKER; SIRNA; IDENTIFICATION; NANOCARRIERS; EXPRESSION; PATTERNS;
D O I
10.1016/j.biomaterials.2016.07.036
中图分类号
R318 [生物医学工程];
学科分类号
0831 ;
摘要
The cancer stem cell (CSC) hypothesis postulates that cancer cells overexpressing CD44 are marked as CSCs that cause tumorigenesis and recurrence. This hypothesis suggests that CD44 is a potential therapeutic target that can interfere with CSCs qualities. MicroRNA-34a (miR-34a) is a promising candidate for CD44 repression-based cancer therapy as it has been reported to inhibit proliferation, metastasis, and survival of CD44-positive CSC5. Here, we used nanovesicles containing PLI/miR complexes (NVs/miR) to systemically deliver miR-34a and induce miR-34a-triggered CD44 suppression in orthotopically and subcutaneously implanted tumors in nude mice. Poly(L-lysine-graft-imidazole) (PLI) condenses miRs and is functionally modified to deliver miRs to the site of action by buffering effect of imidazole residues under endosomal pH. Indeed, NVs/miR consisting of PEGylated lipids enveloping PLI/miR complexes greatly reduced inevitable toxicity of polycations by compensating their surface charge and markedly improved their in vivo stability and accumulation to tumor tissue compared to PLI/miR polyplexes. Our NVs-mediated miR-34a delivery system specifically increased endogenous target miR levels, thereby attenuating proliferation and migration of gastric cancer cells by repressing the expression of CD44 with decreased levels of Bcl-2, Oct 3/4 and Nanog genes. Our strategy led to a greater therapeutic outcome than PLI-based delivery with highly selective tumor cell death and significantly delayed tumor growth in CD44-positive tumor-bearing mouse models, thus providing a fundamental therapeutic window for CSC5. (C) 2016 Elsevier Ltd. All rights reserved.
引用
收藏
页码:12 / 24
页数:13
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