Author/Authors :
Manoochehri, Saeed tehran university of medical sciences tums - Faculty of Pharmacy - Department of Pharmaceutics, تهران, ايران , Darvishi, Behrad tehran university of medical sciences tums - Faculty of Pharmacy - Department of Pharmaceutics, تهران, ايران , Kamalinia, Golnaz tehran university of medical sciences tums - Nanotechnology Research Centre, تهران, ايران , Amini, Mohsen tehran university of medical sciences tums - Faculty of Pharmacy - Department of Medicinal Chemistry, تهران, ايران , Fallah, Mahdieh tehran university of medical sciences tums - Arash Hospital, Faculty of Medicine, تهران, ايران , Ostad, Naser tehran university of medical sciences tums - Faculty of Pharmacy, تهران, ايران , Atyabi, Fatemeh tehran university of medical sciences tums - Faculty of Pharmacy, Nanotechnology Research Centre - Department of Pharmaceutics, تهران, ايران , Dinarvand, Rassoul tehran university of medical sciences tums - Faculty of Pharmacy, Nanotechnology Research Centre - Department of Pharmaceutics, تهران, ايران
Abstract :
Background: Poly lactic-co-glycolic acid (PLGA) based nanoparticles are considered to be a promising drug carrier in tumor targeting but suffer from the high level of opsonization by reticuloendothelial system due to their hydrophobic structure. As a result surface modification of these nanoparticles has been widely studied as an essential step in their development. Among various surface modifications, human serum albumin (HSA) possesses advantages including small size, hydrophilic surface and accumulation in leaky vasculature of tumors through passive targeting and a probable active transport into tumor tissues. Methods: PLGA nanoparticles of docetaxel were prepared by emulsification evaporation method and were surface conjugated with human serum albumin. Fourier transform infrared spectrum was used to confirm the conjugation reaction where nuclear magnetic resonance was utilized for conjugation ratio determination. In addition, transmission electron microscopy showed two different contrast media in conjugated nanoparticles. Furthermore, cytotoxicity of free docetaxel, unconjugated and conjugated PLGA nanoparticles was studied in HepG2 cells. Results: Size, zeta potential and drug loading of PLGA nanoparticles were about 199 nm, −11.07 mV, and 4%, respectively where size, zeta potential and drug loading of conjugated nanoparticles were found to be 204 nm, −5.6 mV and 3.6% respectively. Conjugated nanoparticles represented a three-phasic release pattern with a 20% burst effect for docetaxel on the first day. Cytotoxicity experiment showed that the IC50 of HSA conjugated PLGA nanoparticles (5.4 μg) was significantly lower than both free docetaxel (20.2 μg) and unconjugated PLGA nanoparticles (6.2 μg). Conclusion: In conclusion surface modification of PLGA nanoparticles through HSA conjugation results in more cytotoxicity against tumor cell lines compared with free docetaxel and unconjugated PLGA nanoparticles. Albumin conjugated PLGA nanoparticles may represent a promising drug delivery system in cancer therapy.
Keywords :
PLGA nanoparticles , Surface modification , Human serum albumin , Emulsion evaporation , Tumor targeting , Docetaxel
