Improved Cell Transfection of siRNA by pH-Responsive Nanomicelles Self-Assembled with mPEG-b-PHis-b-PEI Copolymers

Here, the novel pH-responsive nanomicelles self-assembled with amphipathic meo-poly(ethylene glycol)-b-poly(L-histidine)-b-polyethylenimine (mPEG- b-PHis- b-PEI, EHE) copolymers based on hydrophobic interaction of PHis with deprotonation of imidazoles were developed for siRNA transfection. The cationic nanomicelles could electrostatically compact siRNA into stable EHE/siRNA nanoplexes with a hydrodynamic diameter of similar to 190 nm and present a low toxicity in normal physiological condition (pH similar to 7.4). Different from pH-irresponsive ECE/siRNA nanoplexes based on mPEG-b-poly(epsilon-caprolactone)-b-PEI (ECE), the EHE/siRNA nanoplexes exhibited a higher cellular uptake along with an increased zeta-potential (from +18 to +32 mV) when the pH changed from 7.4 to 6.8 (extracellular acidic microenvironments). After cell internalization, the EHE/siRNA nanoplexes also exhibited an enhanced nanostructural disassembling and release of siRNA from lysosomal acidic microenvironments (pH similar to 5.5). Furthermore, it was demonstrated that the EHE/siEGFR nanoplexes downregulated the expression levels of the corresponding mRNA and protein more efficiently than ECE/siEGFR in HeLa cells. The improved siRNA silencing effects of EHE/siEGFR nanoplexes resulted from the higher cellular uptake and enhanced endosomal/lysosomal escape, which is associated with the pH-responsive disassembly of nanostructure as well as the synergistic "proton sponge" effects of PHis and PEI in EHE copolymers. Therefore, the pH-responsive EHE nanomicelles would be promising and potential carriers for cell transfection of siRNA.