In vivo self-assembly and delivery of VEGFR2 siRNA-encapsulated small extracellular vesicles for lung metastatic osteosarcoma therapy

Author:

Yu LingfengORCID,Fan Gentao,Wang Qingyan,Zhu Yan,Zhu Hao,Chang Jiang,Wang Zhen,Zhan Shoubin,Hua Xianming,She Diankun,Huang Jianhao,Wang Yicun,Zhao Jianning,Zhang Chen-YuORCID,Chen XiORCID,Zhou GuangxinORCID

Abstract

AbstractThe prognosis of lung metastatic osteosarcoma (OS) remains disappointing. siRNA-based gene silencing of VEGFR2 is a promising treatment strategy for lung metastatic OS, but there is a lack of safe and efficient delivery systems to encapsulate siRNAs for in vivo administration. This study presented a synthetic biological strategy that remolds the host liver with synthesized genetic circuits for efficient in vivo VEGFR2 siRNA delivery. After being taken-up by hepatocytes, the genetic circuit (in the form of a DNA plasmid) reprogrammed the liver to drive the autonomous intrahepatic assembly and encapsulation of VEGFR2 siRNAs into secretory small extracellular vesicles (sEVs), thus allowing for the transport of self-assembled VEGFR2 siRNAs towards the lung. The results showed that our strategy was superior to the positive medicine (Apatinib) for OS lung metastasis in terms of therapeutic efficacy and toxic adverse effects and may provide a feasible and viable therapeutic solution for lung metastatic OS.

Funder

National Natural Science Foundation of China

Natural Science Foundation of Jiangsu Province

Scientific Research Project of Jiangsu Health Commission

Youth Program of National Natural Science Foundation of China

Publisher

Springer Science and Business Media LLC

Subject

Cancer Research,Cell Biology,Cellular and Molecular Neuroscience,Immunology

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