Functional exosome-mediated co-delivery of doxorubicin and hydrophobically modified microRNA 159 for triple-negative breast cancer therapy

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作者
Chunai Gong
Jing Tian
Zhuo Wang
Yuan Gao
Xin Wu
Xueying Ding
Lei Qiang
Guorui Li
Zhimin Han
Yongfang Yuan
Shen Gao
机构
[1] Changhai Hospital,Department of Pharmaceutics
[2] Second Military Medical University,Department of Pharmacy
[3] Shanghai Ninth People’s Hospital,Department of Clinical Pharmacy and Pharmaceutical Management, School of Pharmacy
[4] Shanghai Jiao Tong University School of Medicine,Department of Clinical Pharmacy, Shanghai General Hospital, School of Medicine
[5] Fudan University,undefined
[6] Shanghai Jiao Tong University,undefined
关键词
Exosome; MicroRNA 159; Doxorubicin; Triple-negative breast cancer; Co-delivery;
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摘要
Exosomes (Exo) hold great promise as endogenous nanocarriers that can deliver biological information between cells. However, Exo are limited in terms of their abilities to target specific recipient cell types. We developed a strategy to isolate Exo exhibiting increased binding to integrin αvβ3. Binding occurred through a modified version of a disintegrin and metalloproteinase 15 (A15) expressed on exosomal membranes (A15-Exo), which facilitated co-delivery of therapeutic quantities of doxorubicin (Dox) and cholesterol-modified miRNA 159 (Cho-miR159) to triple-negative breast cancer (TNBC) cells, both in vitro and in vivo. The targeted A15-Exo were derived from continuous protein kinase C activation in monocyte-derived macrophages. These cell-derived Exo displayed targeting properties and had a 2.97-fold higher production yield. In vitro, A15-Exo co-loaded with Dox and Cho-miR159 induced synergistic therapeutic effects in MDA-MB-231 cells. In vivo, miR159 and Dox delivery in a vesicular system effectively silenced the TCF-7 gene and exhibited improved anticancer effects, without adverse effects. Therefore, our data demonstrate the synergistic efficacy of co-delivering miR159 and Dox by targeted Exo for TNBC therapy.
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