Release mechanisms of tacrolimus-loaded PLGA and PLA microspheres and immunosuppressive effects of the microspheres in a rat heart transplantation model

他克莫司 PLGA公司 化学 药理学 吸收(声学) 药代动力学 剂型 移植 毒品携带者 色谱法 医学 材料科学 外科 生物化学 药品 体外 复合材料
作者
Ryo Kojima,Tsuneya Yoshida,Hiroaki Tasaki,Hiroyuki Umejima,Masashi Maeda,Yasuyuki Higashi,Susumu Watanabe,Naoto Oku
出处
期刊:International Journal of Pharmaceutics [Elsevier]
卷期号:492 (1-2): 20-27 被引量:23
标识
DOI:10.1016/j.ijpharm.2015.07.004
摘要

The objective of this study was to elucidate the release and absorption mechanisms of tacrolimus loaded into microspheres composed of poly(lactic-co-glycolic acid) (PLGA) and/or polylactic acid (PLA). Tacrolimus-loaded microspheres were prepared by the o/w emulsion solvent evaporation method. The entrapment efficiency correlated with the molecular weight of PLGA, and the glass transition temperature of PLGA microspheres was not decreased by the addition of tacrolimus. These results indicate that intermolecular interaction between tacrolimus and the polymer would affect the entrapment of tacrolimus in the microspheres. Tacrolimus was released with weight loss of the microspheres, and the dominant release mechanism of tacrolimus was considered to be erosion of the polymer rather than diffusion of the drug. The whole-blood concentration of tacrolimus in rats was maintained for at least 2 weeks after a single subcutaneous administration of the microspheres. The pharmacokinetic profile of tacrolimus following subcutaneous administration was similar to that following intramuscular administration, suggesting that the release and dissolution of tacrolimus, rather than the absorption of the dissolved tacrolimus, were rate-limiting steps. Graft-survival time in a heart transplantation rat model was prolonged by the administration of tacrolimus-loaded microspheres. The microsphere formulation of tacrolimus would be expected to precisely control the blood concentration while maintaining the immunosuppressive effect of the drug.
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