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Facile fabrication of PEG-coated PLGA microspheres via SPG membrane emulsification for the treatment of scleroderma by ECM degrading enzymes

机译:通过SPG膜乳化通过ECM降解酶处理PEG涂覆的PLGA微球的化妆术治疗硬皮病治疗SCLODERMA

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摘要

We developed a facile fabrication method for preparing poly(ethylene glycol)(PEG)-coated poly (lactic-co-glycolic acid) (PLGA) microspheres with homogeneous size distribution via a combination of mPEG-b-PLGA and Shirasu Porous Glass membrane emulsification. Subsequently, extracellular matrix (ECM) degrading enzymes, collagenase (COLase) or hyaluronidase (HAse) were loaded into the microspheres. The obtained microspheres exhibited a sustained release of COLase or HAse over 10 days. The degradation of ECM polymers by the released COLase and HAse was confirmed in vitro. Reversal of established dermal fibrosis via degradation of over-deposited ECM is a promising treatment for scleroderma. The therapeutic effects of COLase- and HAse-loaded PLGA microspheres on scleroderma were evaluated in vivo following their intradermal administration to a bleomycin-induced mice model of scleroderma. COLase- and HAse-loaded PLGA microspheres decreased scleroderma dermal thickness without altering the mechanical properties of skin, whereas the administration of free COLase and HAse solution induced overdecomposition of skin ECM and alpha-SMA expression. The facile one-pot synthesis of PEG-coated PLGA microspheres with high colloidal stability and narrow size distribution could be employed as a drug carrier for various diseases in future.
机译:我们开发了一种用于制备聚(乙二醇)(PEG)涂覆的聚(乳酸二乙醇酸)(PLGA)微球的容易制造方法,通过MPEG-B-PLGA和Shirasu多孔玻璃膜乳化的组合进行均匀尺寸分布。随后,将细胞外基质(ECM)降解酶,胶原酶(Colase)或透明质酸酶(Hase)加载到微球中。所获得的微球在10天内表现出Colase或Hase的持续释放。通过释放的Coolase和Hase的ECM聚合物的降解在体外证实。通过过度沉积的ECM降解已建立的皮肤纤维化的逆转是硬皮病的有希望的治疗方法。在其皮内给药到晶体霉素诱导的硬皮病模型之后,在体内评估CORAPE-和HASE-HARE-HARGA MICROMA对硬皮病的治疗效果。加载的PLGA微球降低了硬皮病的皮肤厚度,而不改变皮肤的机械性能,而游离的Carase和HASE溶液的给药诱导过度分解皮肤ECM和α-SMA表达。具有高胶体稳定性和窄尺寸分布的PEG涂覆的PLGA微球的容易单壶合成可用于未来各种疾病的药物载体。

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