PLGA microsphere/PVA hydrogel coatings suppress the foreign body reaction for 6 months

被引:45
作者
Gu, Bing [1 ]
Papadimitrakopoulos, Fotios [1 ]
Burgess, Diane J. [1 ]
机构
[1] Univ Connecticut, Sch Pharm, Storrs, CT 06269 USA
基金
美国国家科学基金会;
关键词
Polymer blends; Heat map; Dose response; Long-term; PLGA microsphere; DIABETIC MACULAR EDEMA; DEXAMETHASONE INTRAVITREAL IMPLANT; IN-VIVO; POLYURETHANE COATINGS; INSULIN ABSORPTION; GLUCOSE SENSORS; POLYMER BLENDS; RELEASE; ANGIOGENESIS; PERFORMANCE;
D O I
10.1016/j.jconrel.2018.09.021
中图分类号
O6 [化学];
学科分类号
0703 ;
摘要
The application of dexamethasone releasing poly (lactic-co-glycolic acid) (PLGA) microspheres embedded in a poly vinyl alcohol (PVA) hydrogel coatings have been successfully used in the suppression of the foreign body response (FBR) to implantable glucose sensors. In the current study, dexamethasone-loaded PLGA microspheres were prepared by blending two types of PLGA polymers (RG503H and DLG7E with MW of ca. 25 kDa and 113 kDa, respectively) to achieve long-term (6 months) inhibition of the FBR. The microsphere composition was optimized according to the in vitro drug release profiles. Microspheres with DLG7E/RG503H/dexamethasone = 70/13.3/16.7 wt% composition, when embedded in a PVA hydrogel, provided a continuous drug release for 6 months. By combining the aforementioned microspheres with microspheres composed solely of the DLG7E polymer within a similar PVA hydrogel realized an even longer (> 7 months) in vitro drug release. A heat map was constructed to depict the daily in vitro drug released and elucidate possible lag phases that could affect the pharmacodynamic response. These drug-loaded implant coatings were investigated in vivo (rat model) and showed inhibition of the foreign body response for 6 months. These results suggest that the minimum effective daily dose to counter chronic inflammation is ca. 0.1 mu g per mg of coating surrounding a 0.5 x 0.5 x 5 mm silicon implant (dummy sensor). Accordingly, these drug-eluting composite coatings can ensure long-term inflammation control for miniaturized implantable devices.
引用
收藏
页码:35 / 43
页数:9
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