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Merck

Polyphosphoester nanoparticles as biodegradable platform for delivery of multiple drugs and siRNA.

Drug design, development and therapy (2017-03-07)
Hadeel Elzeny, Fuwu Zhang, Esraa N Ali, Heba A Fathi, Shiyi Zhang, Richen Li, Mohamed A El-Mokhtar, Mostafa A Hamad, Karen L Wooley, Mahmoud Elsabahy
ABSTRAKT

Delivery of multiple therapeutics and/or diagnostic agents to diseased tissues is challenging and necessitates the development of multifunctional platforms. Among the various strategies for design of multifunctional nanocarriers, biodegradable polyphosphoester (PPE) polymers have been recently synthesized via a rapid and simple synthetic strategy. In addition, the chemical structure of the polymer could be tuned to form nanoparticles with varying surface chemistries and charges, which have shown exceptional safety and biocompatibility as compared to several commercial agents. The purpose of this study was to exploit a mixture of PPE nanoparticles of cationic and neutral surface charges for multiple delivery of anticancer drugs (ie, sorafenib and paclitaxel) and nucleic acids (ie, siRNA). Cationic PPE polymers could efficiently complex siRNA, and the stability of the nanoparticles could be maintained in physiological solutions and upon freeze-drying and were able to deliver siRNA in vivo when injected intravenously in mice. Commercially available cationic polyethylenimine polymer had LD

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Sigma-Aldrich
2-Phenylacetophenone, 97%