Local delivery of controlled-release simvastatin/PLGA/HAp microspheres enhances bone repair

辛伐他汀 PLGA公司 药理学 骨愈合 洛伐他汀 体内 新生血管 化学 医学 生物医学工程 体外 外科 内科学 血管生成 胆固醇 生物化学 生物 生物技术
作者
Mei‐Ling Ho,Tai Tai,Fu,Chih‐Kuang Wang,Chang
出处
期刊:International Journal of Nanomedicine [Dove Medical Press]
卷期号:: 3895-3895 被引量:93
标识
DOI:10.2147/ijn.s48694
摘要

Abstract: Statins are used clinically for reduction of cholesterol synthesis to prevent cardiovascular disease. Previous in vitro and in vivo studies have shown that statins stimulate bone formation. However, orally administered statins may be degraded during first-pass metabolism in the liver. This study aimed to prevent this degradation by developing a locally administered formulation of simvastatin that is encapsulated in poly(lactic-co-glycolic acid)/hydroxyapatite (SIM/PLGA/HAp) microspheres with controlled-release properties. The effect of this formulation of simvastatin on bone repair was tested using a mouse model of gap fracture bridging with a graft of necrotic bone. The simvastatin released over 12 days from 3 mg and 5 mg of SIM/PLGA/HAp was 0.03–1.6 µg/day and 0.05–2.6 µg/day, respectively. SIM/PLGA/HAp significantly stimulated callus formation around the repaired area and increased neovascularization and cell ingrowth in the grafted necrotic bone at week 2 after surgery. At week 4, both 3 mg and 5 mg of SIM/PLGA/HAp increased neovascularization, but only 5 mg SIM/PLGA/HAp enhanced cell ingrowth into the necrotic bone. The low dose of simvastatin released from SIM/PLGA/HAp enhanced initial callus formation, neovascularization, and cell ingrowth in the grafted bone, indicating that SIM/PLGA/HAp facilitates bone regeneration. We suggest that SIM/PLGA/HAp should be developed as an osteoinductive agent to treat osteonecrosis or in combination with an osteoconductive scaffold to treat severe bone defects. Keywords: statin, controlled release, poly(lactic-co-glycolic acid), microspheres, bone fracture
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