Nintedanib-cyclodextrin complex to improve bio-activity and intestinal permeability

•Cyclodextrin inclusion complex of nintedanib prepared using different cyclodextrins.•Sulfobutyl ether β-CD demonstrated higher inclusion and better stability.•Inclusion complex improved transport across clinically relevant EpiIntestinal tissue model.•Inclusion complex also improved bio-activity of nintedanib against lung fibroblast cells.•Shows promise to use via oral or pulmonary route in novel dosage forms. Cyclodextrin complex of nintedanib was prepared aiming for increased bio-activity and improved transport across intestinal membrane with reduced p-glycoprotein (p-gp) efflux. Based on preliminary phase solubility studies and molecular modeling, sulfobutyl ether derivative of β-cyclodextrin (SBE-β-CD, Captisol®) was selected to prepare inclusion complex. Complexation was confirmed using FTIR, 1H NMR, DSC, and XRD. Bioactivity of the formed complex was tested using lung fibroblast cells, WI-38 for anti-proliferative activity and effect on collagen deposition and cells migration. In-vitro permeability studies were performed using epiIntestinal tissue model to assess the effect of complexation on transport and p-gp efflux. Results of the study demonstrated that cyclodextrin complexation increased stability of nintedanib in PBS (pH 7.4) and simulated intestinal fluid (SIF). Further, bioactivity of nintedanib also improved. Interestingly, complexation has increased transport of nintedanib across intestinal membrane and reduced efflux ratio, suggesting the role of cyclodextrin complexation in modulating p-gp efflux.