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Prolonging the plasma circulation of proteins by nano- encapsulation with phosphorylcholine-based polymer 被引量:4
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作者 Linlin Zhang Yang Liu +5 位作者 Gan Liu Duo Xu Sheng Liang Xinyuan Zhu Yunfeng Lu Hui Wang 《Nano Research》 SCIE EI CAS CSCD 2016年第8期2424-2432,共9页
Short in vivo circulation is a major hindrance to the widespread adoption of protein therapeutics. Protein nanocapsules generated by encapsulating proteins with a thin layer of phosphorylcholine-based polymer via a tw... Short in vivo circulation is a major hindrance to the widespread adoption of protein therapeutics. Protein nanocapsules generated by encapsulating proteins with a thin layer of phosphorylcholine-based polymer via a two-step encapsulation process exhibited significantly prolonged plasma half-life. Furthermore, by constructing nanocapsules with similar sizes but different surface charges and chemistry, we demonstrated a generic strategy for prolonging the plasma half-life of therapeutic proteins. In an in vitro experiment, four types of bovine serum albumin (BSA) nanocapsules were incubated with fetal bovine serum (FBS) in phosphate buffer saline (PBS); the cell uptake by HeLa cells was monitored to systematically evaluate the characteristics of the surface chemistry during drculation. Single positron emission tomography-computed tomography (SPECT) was employed to allow real-time observation of the BSA nanoparticle distribution in vivo, as well as quantification of the plasma concentration after intravenous administration. This study offers a practical method for translating a broad range of proteins for clinical use. 展开更多
关键词 phosphorylcholine-basedpolymer nano-encapsulation function protein delivery protein therapy long-circulation
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