The physical sorption of a series of cyclophosPhamide drug derivatives with formula [NH(CH2)(3)O]P(O)(N[(CH2)(x)X](2)) where x = 2, X = F (2), Cl (3), Br (4); x=3, X=F (5), Cl (6), Br (7) and x =4, X = F (8), Cl (9), Br (10) on the surface of fullerene C-60 was studied using density functional theory (DFT) at B3LYP and B3PW91 levels. The most negative binding energies obtained using the B3LYP approach and corrected for geometrical BSSE and dispersion energies (gCP-D3-Delta E-binding) were measured for compounds 8 (among isolated drugs) and 13 (among complexes). The dipole moments of isolated drugs were obtained close to those of their complexes with C-60 (similar to 4.0-5.5 Debye) indicating their hydrophililic nature that is an appropriate property appealing for drug delivery in biological media. The adsorption of all drugs on the surface of fullerene was endergonic with all of the Delta G(adsorption) %26gt; 0. The Delta H-adsorption values at B3PW91 level were only negative for complexes 14-16 indicating their exothermic adsorption nature. The HOMO-LUMO band gaps of complexes 11-19 were about 2.7 eV and are comparable with the gap in C-60 but are much smaller than the gaps in isolated drugs 2-10 (6.5-8.0 eV) reflecting the increase in electrical conductivities upon complexation. The QTAIM data supported the covalent character of the C-O, C-N and N-H bonds, the intermediate character of P=O, P-O and P-N bonds while the electrostatic nature of P=O center dot center dot center dot C(fullerene) interactions. According to the gCP-D3-Delta E-binding binding energies and Delta H-adsorption values at B3LYP level, it seems that the complexes 12 and 13 can be the most promising prodrug + carrier delivery systems.

• 出版日期2014-7