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聚(乙基丙烯酸)的烷基化衍生物可插入预先形成的脂质体中,并触发脂质体内容物的pH依赖性细胞内递送。

Alkylated derivatives of poly(ethylacrylic acid) can be inserted into preformed liposomes and trigger pH-dependent intracellular delivery of liposomal contents.

作者信息

Chen Tao, McIntosh Deirdre, He Yuehua, Kim Jungsoo, Tirrell David A, Scherrer Peter, Fenske David B, Sandhu Ammen P, Cullis Pieter R

机构信息

Department of Biochemistry and Molecular Biology, University of British Columbia, Vancouver, BC, V6T 1Z3, Canada.

出版信息

Mol Membr Biol. 2004 Nov-Dec;21(6):385-93. doi: 10.1080/09687860400010516.

DOI:10.1080/09687860400010516
PMID:15764368
Abstract

Poly(ethylacrylic acid) (PEAA) is a pH-sensitive polymer that undergoes a transition from a hydrophilic to a hydrophobic form as the pH is lowered from neutral to acidic values. In this work we show that pH sensitive liposomes capable of intracellular delivery can be constructed by inserting a lipid derivative of PEAA into preformed large unilamellar vesicles (LUV) using a simple one step incubation procedure. The lipid derivatives of PEAA were synthesized by reacting a small proportion (3%) of the carboxylic groups of PEAA with C10 alkylamines to produce C10-PEAA. Incubation of C10-PEAA with preformed LUV resulted in the association of up to 8% by weight of derivatized polymer with the LUV without inducing aggregation. The resulting C10-PEAA-LUV exhibited pH-dependent fusion and leakage of LUV contents on reduction of the external pH below pH 6.0 as demonstrated by lipid mixing and release of calcein encapsulated in the LUV. In addition, C10-PEAA-LUV exhibited pH dependent intracellular delivery properties following uptake into COS-7 cells with appreciable delivery to the cell cytoplasm as evidenced by the appearance of diffuse intracellular calcein fluorescence. It is demonstrated that the cytoplasmic delivery of calcein by C10-PEAA-LUV could be inhibited by agents (bafilomycin or chloroquine) that inhibit acidification of endosomal compartments, indicating that this intracellular delivery resulted from the pH-dependent destabilization of LUV and endosomal membranes by the PEAA component of the C10-PEAA-LUV. It is concluded that C10-PEAA-LUV represents a promising intracellular delivery system for in vitro and in vivo applications.

摘要

聚(乙基丙烯酸)(PEAA)是一种对pH敏感的聚合物,当pH从中性降低到酸性值时,它会从亲水性形式转变为疏水性形式。在这项工作中,我们表明,通过使用简单的一步孵育程序将PEAA的脂质衍生物插入预先形成的大单层囊泡(LUV)中,可以构建能够进行细胞内递送的pH敏感脂质体。PEAA的脂质衍生物是通过使少量(3%)的PEAA羧基与C10烷基胺反应生成C10-PEAA来合成的。将C10-PEAA与预先形成的LUV孵育,导致高达8%(重量)的衍生聚合物与LUV结合,而不会诱导聚集。所得的C10-PEAA-LUV在外部pH降低至6.0以下时表现出pH依赖性的LUV内容物融合和泄漏,这通过脂质混合和LUV中封装的钙黄绿素的释放得到证明。此外,C10-PEAA-LUV在被COS-7细胞摄取后表现出pH依赖性的细胞内递送特性,有相当数量的物质递送至细胞质,这通过弥漫性细胞内钙黄绿素荧光的出现得到证明。结果表明,C10-PEAA-LUV介导的钙黄绿素向细胞质的递送可被抑制内体区室酸化的试剂(巴弗洛霉素或氯喹)抑制,这表明这种细胞内递送是由于C10-PEAA-LUV的PEAA组分对LUV和内体膜的pH依赖性破坏所致。结论是,C10-PEAA-LUV代表了一种用于体外和体内应用的有前景的细胞内递送系统。

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