In vitro and in vivo studies of cyclosporin A-loaded microspheres based on copolymers of lactide and ɛ-caprolactone: Comparison with conventional PLGA microspheres

Abstract

A hydrophobic peptide, cyclosporin A (CyA), was incorporated in microspheres based on poly(lactide- b-ɛ-caprolactone) (P(LA- b-CL), LA/CL (in molar ratio): 78.7/21.3 and 48.1/51.9) and poly(lactide-co-glycolide) (PLGA, LA/GA: 80/20) using oil-in-water (O/W) emulsion solvent evaporation method. The microspheres were characterized by SEM, DSC and X-ray diffraction, and CyA release rate was determined by HPLC. It was revealed that CyA can be efficiently loaded into all the microspheres (exceed 96%). Compared to PLGA microspheres, P(LA- b-CL) microspheres liberated CyA more rapidly. Within the first day, about 75, 50 and 12% of CyA released from P(LA- b-CL) (48.1/51.9), P(LA- b-CL) (78.7/21.3) and PLGA microspheres, respectively, which can be attributed to the partial crystallization occurring in P(LA- b-CL) microspheres. CyA levels in whole blood were also tested. In comparison with PLGA microspheres, P(LA- b-CL) microspheres provided a higher blood level of CyA. The maximum CyA concentration in whole blood (∼520, 450 and 400 ng ml −1 for P(LA- b-CL) (48.1/51.9) P(LA- b-CL) (78.7/21.3) and PLGA microspheres, respectively) was reached at the second day post administration. And then P(LA- b-CL) microspheres showed a constant CyA level (about 100–200 ng ml −1) for extended periods of time (several weeks). Such CyA-loaded P(LA- b-CL) microspheres displaying higher CyA concentration during the first few days and similar constant blood CyA level thereafter showed more advantages than those prepared with PLGA and could meet clinical needs more efficiently.