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Beta-cyclodextrin modified mesoporous bioactive glass nanoparticles/silk fibroin hybrid nanofibers as an implantable estradiol delivery system for the potential treatment of osteoporosis

机译:Beta-cyclodextrin改性介孔生物活性玻璃/丝素蛋白纳米颗粒混合纳米纤维作为一种植入式雌二醇交付系统的潜在的治疗骨质疏松症

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摘要

Osteoporosis, a systemic skeletal disease prevalent in elderly women, is associated with post-menopausal estrogen deficiency. Although systemic administration of exogenous estradiol (E2) reduced fragility fractures, the treatment has adverse effects. Localized delivery technologies of E2 could be utilized to circumvent the systemic adverse effects of systemic administration. In this study, a localized E2 delivery system is developed. Mesoporous bioactive glass nanoparticles (MBGNPs) with inherent osteogenic properties are modified with -cyclodextrin (CD-MBGNPs) to enhance their affinity for E2. To ensure mechanical stability and integrity, E2 loaded CD-MBGNPs are further electrospun with silk fibroin (SF) to produce a nanofibrous mesh (E2@CD-MBGNPs/SF). The incorporation of MBGNPs in SF enhances in vitro apatite formation and sustains the constant release of E2. Moreover, osteoblast proliferation and differentiation markers such as alkaline phosphatase activity, collagen 1 and osteocalcin expression of MC3T3-E1 are augmented in CD-MBGNPs/SF and E2@CD-MBGNPs/SF as compared to SF nanofibers. On the other hand, osteoclast DNA, tartrate resistant acid phosphatase activity and multinucleated cell formation are reduced in E2@CD-MBGNPs/SF as compared to CD-MBGNPs/SF and SF. Hence the presence of CD-MBGNPs in SF stimulates osteoblast function whereas E2 incorporation in CD-MBGNPs/SF reduces osteoclast activity. This is the first report to develop CD-MBGNPs/SF as a localized delivery system for hydrophobic molecules such as estradiol to treat osteoporosis.
机译:骨质疏松症,一种全身性骨骼疾病在老年女性普遍,是联系在一起的绝经后雌激素缺乏症。系统性的管理外生雌二醇(E2)减少脆弱性骨折,治疗有不利影响。E2可以利用的技术规避系统性不良反应系统性的管理。本地化E2交付系统。介孔生物活性玻璃纳米颗粒(MBGNPs)与成骨的固有属性修改与环糊精(CD-MBGNPs)来提高自己E2的亲和力。和完整性,E2 CD-MBGNPs进一步加载实际上电纺与丝素蛋白(SF)生产nanofibrous网(E2@CD-MBGNPs / SF)。整合MBGNPs科幻提高体外磷灰石形成和维持不变E2的释放。和分化标记如碱性磷酸酶活性,胶原蛋白1和骨钙蛋白MC3T3-E1的表达增强CD-MBGNPs /科幻和E2@CD-MBGNPs /科幻相比科幻小说纳米纤维。抗酒石酸酸性磷酸酶活性和多核细胞形成减少E2@CD-MBGNPs / CD-MBGNPs /科幻小说和科幻小说相比科幻小说。而E2刺激成骨细胞功能合并CD-MBGNPs /科幻减少破骨细胞活动。CD-MBGNPs /科幻作为一个局部的交付系统疏水性分子如雌二醇治疗骨质疏松症。

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