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Block Copolymer Micelles as Nanocontainers for Controlled Release of Proteins from Biocompatible Oil Phases

机译:嵌段共聚物胶束作为纳米容器用于从生物相容性油相中控制释放蛋白质

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摘要

Biocompatible oils are used in a variety of medical applications ranging from vaccine adjuvants to vehicles for oral drug delivery. To enable such nonpolar organic phases to serve as reservoirs for delivery of hydrophilic compounds, we explored the ability of block copolymer micelles in organic solvents to sequester proteins for sustained release across an oil−water interface. Self-assembly of the block copolymer, poly(ϵ-caprolactone)-block-poly(2-vinyl pyridine) (PCL-b-P2VP), was investigated in toluene and oleic acid, a biocompatible naturally occurring fatty acid. Micelle formation in toluene was characterized by dynamic light scattering (DLS) and atomic force microscopy (AFM) imaging of micelles cast onto silicon substrates. Cryogenic transmission electron microscopy confirmed a spherical morphology in oleic acid. Studies of homopolymer solubility implied that micelles in oleic acid consist of a P2VP corona and a PCL core, while P2VP formed the core of micelles assembled in toluene. The loading of two model proteins (ovalbumin (ova) and bovine serum albumin (BSA)) into micelles was demonstrated with loadings as high as 7.8% wt of protein per wt of P2VP in oleic acid. Characterization of block copolymer morphology in the two solvents after protein loading revealed spherical particles with similar size distributions to the as-assembled micelles. Release of ova from micelles in oleic acid was sustained for 12−30 h upon placing the oil phase in contact with an aqueous bath. Unique to the situation of micelle assembly in an oily phase, the data suggest protein is sequestered in the P2VP corona block of PCL-b-P2VP micelles in oleic acid. More conventionally, protein loading occurs in the P2VP core of micelles assembled in toluene.
机译:生物相容性油用于各种医疗应用,从疫苗佐剂到用于口服药物递送的载体。为了使此类非极性有机相能够用作亲水性化合物的输送库,我们探索了有机溶剂中嵌段共聚物胶束螯合蛋白质以跨油水界面持续释放的能力。在甲苯和油酸(一种生物相容性天然脂肪酸)中研究了嵌段共聚物聚(ε-己内酯)-嵌段-聚(2-乙烯基吡啶)(PCL-b-P2VP)的自组装。甲苯中胶束的形成是通过动态光散射(DLS)和浇铸在硅基板上的胶束的原子力显微镜(AFM)成像来表征的。低温透射电子显微镜证实油酸呈球形。对均聚物溶解度的研究表明,油酸中的胶束由P2VP电晕和PCL核组成,而P2VP则形成了组装在甲苯中的胶束核。两种模型蛋白(卵清蛋白(ova)和牛血清白蛋白(BSA))在胶束中的负载量高达每重量P2VP油酸中7.8%的负载量。加载蛋白质后,两种溶剂中嵌段共聚物的形态表征表明球形颗粒的大小分布与组装的胶束相似。将油相与水浴接触后,在油酸中的胶束中的卵释放持续12-30小时。对于油相中的胶束组装情况而言,独特的数据表明蛋白质被隔离在油酸中的PCL-b-P2VP胶束的P2VP电晕嵌段中。更常规地,蛋白质负载发生在组装在甲苯中的胶束的P2VP核心中。

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