Electrical-charge mediated cancer cell targeting via protein corona decorated superparamagnetic nanoparticles in simulated physiological environment.

A critical issue in nanomedicine is on the understanding of nano-bio interface behaviors, particularly when the nanoparticles are inevitably decorated by protein coronas in the physiological fluids. In this study, the effects of particle surface corona on cancer cell targeting were investigated in simulated physiological fluids. Cell targeting was achieved by two strategies: (1) using conventional EpCAM antibody-functionalized Fe3O4 nanoparticles, and (2) rendering the same but naked magnetic nanoparticles electrically-positively charged enabling them to electrostatically bind onto the negatively-charged cancer cells. The cell-particle electrostatic binding was found much stronger with faster reaction kinetics than the immunological interactions even at 4 ̊C. Both types of nanoparticles were decorated with various protein coronas by administration in a simulated physiological system. Well-decorated by protein coronas, the electrically-charged particles retained strong electrostatic interactions with cancer cells, even upon reversal of the particle Zeta potential from positive to negative. This behavior was explained by a non-uniform corona modulation of the particle surface charge distributions, exposing locally positively-charged regions, capable of strong electrostatic cell binding and magnetic capturing in a physiological environment. This fundamental discovery paves a new way for sensitive detection of circulating tumor cells in whole blood in clinical settings.