Abstract
•Binding of drug with metal ions has been investigated by UV–visible/DFT studies.•Binding constant values for transition metal showed order: Cu2+ > Ni2+ > Co2+ > Zn2+.•Study suggests hydrophobic interactions for binding of drug with alkali earth metal.•Herein, electrostatic/ion–dipole/H-bonding interactions are recommended.•Bond lengths, bond angles, etc. of drug/drug-metal ion complexes are calculated from DFT study.
Herein, we have studied the binding of levofloxacin hemihydrate (LFH) drug with different metal ions e.g., alkali earth metal ions and transition metal ions through spectrophotometry and Density Function Theory (DFT) studies. The binding constant (Kf) of LFH with alkali earth metal ions was observed to be increased with the boost of temperature while the opposite trend was observed in the case of transition metal ions. The Kf values were experienced to be reduced with the increase of size of the alkali earth metal ions. The Kf values in case of transition metal follow the order Cu2+ > Ni2+ > Co2+ > Zn2+. The Gibbs free energy (ΔG0) of binding values reveal that binding phenomena are spontaneous in nature. The values of enthalpy (ΔH0) and entropy (ΔS0) of binding suggest that hydrophobic interactions are the key forces for the binding of LFH and alkali earth metal ions while electrostatic, dipole-dipole, ion-dipole, and hydrogen bonding are the key forces in case of transition metal ions. The enthalpy-entropy compensation parameters were also estimated and explained in detail. From the DFT study, the bond lengths, bond angles, HOMO and LUMO orbitals energy, band gap, hardness, and the highest wavelengths of the drug/ drug-metal complexes have been calculated and explained with appropriate reasoning.