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Autologous platelet delivery of siRNAs by autologous plasma protein self-assembled nanoparticles for the treatment of acute kidney injury

Journal of nanobiotechnology. 2014-04; 
Jiafan Wang; Hai Huang; Meng Jia; Si Chen; Fengjuan Wang; Guiyang He; Chong Wu; Kaibin Lou; Xuexue Zheng; Heng Zhang; Chao Qin; Yanggang Yuan; Ke Zen; Hongwei Liang
Products/Services Used Details Operation
Gene Synthesis fluorophore attached at the 5 -terminus) or naked scramble RNA (siRNA-NC), TP53 siRNA and Trp53 siRNAs (siRNA-Trp53) were 2 -O-methylated and synthesized by GenScript (Nanjing, China). The reverse complementary sequence of siRNA-TP53 (siRNA-TP53 inhibitor) was synthesized by GenePharma (Shanghai, China). Cisplatin Get A Quote

摘要

Acute kidney injury (AKI) involves the activation of intrarenal hemostatic and inflammatory pathways. Platelets rapidly migrate to affected sites of AKI and release extracellular vesicles (EVs) laden with bioactive mediators that regulate inflammation and hemostasis. While small interfering RNA (siRNA) is a potent gene-silencing tool for biomedical applications, its therapeutic application in vivo remains challenging. We developed an innovative nucleic acid delivery platform by hybridizing synthetic transformation-related protein 53 (p53) siRNA with autologous plasma and incubating the complex with autologous platelets. These engineered platelets selectively delivered p53 siRNA to injured renal tubular cells vi... More

关键词

Acute kidney injury, Platelets, Self-assembling nanoparticles, Transformation-related protein 53