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胆固醇介导的载酶脂质体在二硫键稳定的聚合物载体胶囊内的锚定。

Cholesterol-mediated anchoring of enzyme-loaded liposomes within disulfide-stabilized polymer carrier capsules.

作者信息

Chandrawati Rona, Städler Brigitte, Postma Almar, Connal Luke A, Chong Siow-Feng, Zelikin Alexander N, Caruso Frank

机构信息

Centre for Nanoscience and Nanotechnology, Department of Chemical and Biomolecular Engineering, The University of Melbourne, Parkville, Victoria, Australia.

出版信息

Biomaterials. 2009 Oct;30(30):5988-98. doi: 10.1016/j.biomaterials.2009.07.040. Epub 2009 Aug 15.

DOI:10.1016/j.biomaterials.2009.07.040
PMID:19683341
Abstract

Polymer capsules containing multiple liposomes, termed capsosomes, are a promising new concept toward the design of artificial cells. Herein, we report on the fundamental aspects underpinning the assembly of capsosomes. A stable and high loading of intact liposomal cargo into a polymer film was achieved by non-covalently sandwiching the liposomes between a tailor-made cholesterol-modified poly(L-lysine) (PLL(c)) precursor layer and a poly(methacrylic acid)-co-(cholesteryl methacrylate) (PMA(c)) capping layer. The film assembly, optimized on planar surfaces, was successfully transferred onto colloidal substrates, and a polymer membrane was subsequently assembled by the alternating adsorption of poly(N-vinyl pyrrolidone) (PVP) and thiol-modified poly(methacrylic acid) (PMA(SH)) onto the pre-adsorbed layer of liposomes. Upon removal of the silica template, stable capsosomes encapsulating the enzyme luciferase or beta-lactamase within their liposomal sub-compartments were obtained at both assembly (pH 4) and physiological conditions (pH 7.4). Excellent retention of the liposomes and the enzymatic cargo within the polymer carrier capsules was observed for up to 14 days. These engineered capsosomes are particularly attractive as autonomous microreactors, which can be utilized to repetitively add smaller reactants to cause successive distinct reactions within the capsosomes and simultaneously release the products to the surrounding environment, bringing these systems one step closer toward constructing artificial cells.

摘要

包含多个脂质体的聚合物胶囊,即所谓的囊体,是人工细胞设计方面一个很有前景的新概念。在此,我们报告囊体组装的基本原理。通过将脂质体非共价夹在特制的胆固醇修饰聚(L-赖氨酸)(PLL(c))前体层和聚(甲基丙烯酸)-共-(甲基丙烯酸胆固醇酯)(PMA(c))封端层之间,实现了完整脂质体货物在聚合物膜中的稳定高负载。在平面表面优化后的膜组装成功转移到胶体基质上,随后通过聚(N-乙烯基吡咯烷酮)(PVP)和硫醇修饰的聚(甲基丙烯酸)(PMA(SH))交替吸附到预先吸附的脂质体层上组装聚合物膜。去除二氧化硅模板后,在组装时(pH 4)和生理条件下(pH 7.4)均获得了在其脂质体子隔室内封装荧光素酶或β-内酰胺酶的稳定囊体。在聚合物载体胶囊内,脂质体和酶货物的保留率高达14天。这些工程化囊体作为自主微反应器特别有吸引力,可用于重复添加较小的反应物,在囊体内引发连续的不同反应,并同时将产物释放到周围环境中,使这些系统向构建人工细胞迈进了一步。

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