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在单脂质体水平定量药物递送脂质体的组成不均匀性。

Compositional inhomogeneity of drug delivery liposomes quantified at the single liposome level.

作者信息

Andresen Thomas Lars, Larsen Jannik Bruun

机构信息

Center for Nanomedicine and Theranostics, Center for Intestinal Absorption and Transport of Biopharmaceuticals, Department of Health Technology, Technical University of Denmark, DK-2800, Kgs. Lyngby, Denmark.

Center for Nanomedicine and Theranostics, Center for Intestinal Absorption and Transport of Biopharmaceuticals, Department of Health Technology, Technical University of Denmark, DK-2800, Kgs. Lyngby, Denmark.

出版信息

Acta Biomater. 2020 Dec;118:207-214. doi: 10.1016/j.actbio.2020.10.003. Epub 2020 Oct 14.

Abstract

Liposomes are the most used drug delivery vehicle and their therapeutic function is closely linked to their lipid composition. Since most liposome characterization is done using bulk techniques, providing only ensemble averages, the lipid composition of all liposomes within the same formulation are typically assumed to be identical. Here we image individual liposomes using confocal microscopy to quantify that liposomal drug delivery formulations, including multiple component mixtures mimicking Doxil, display more than 10-fold variation in their relative lipid composition. Since liposome function is tightly regulated by the physicochemical properties bestowed by the lipid composition, such significant variations could render only a fraction of liposomes therapeutically active. Additionally, we quantified how this degree of compositional inhomogeneity was modulated by liposome preparation method, the saturation state of the membrane lipid, and whether anti-fouling polyethylene glycol (PEG) conjugated lipids were added to the initial lipid mix or inserted after liposome formation. We believe the insights into the factors governing the degree of inhomogeneity offers the possibility for producing more uniform liposomal drug delivery systems, potentially increasing their therapeutic efficacy.

摘要

脂质体是最常用的药物递送载体,其治疗功能与其脂质组成密切相关。由于大多数脂质体表征是使用整体技术进行的,仅提供总体平均值,因此通常假定同一制剂中所有脂质体的脂质组成是相同的。在这里,我们使用共聚焦显微镜对单个脂质体进行成像,以量化脂质体药物递送制剂,包括模拟多柔比星脂质体(Doxil)的多组分混合物,其相对脂质组成显示出超过10倍的变化。由于脂质体功能受脂质组成赋予的物理化学性质严格调控,这种显著变化可能仅使一小部分脂质体具有治疗活性。此外,我们量化了这种组成不均匀程度是如何受到脂质体制备方法、膜脂饱和状态以及抗污聚乙二醇(PEG)共轭脂质是添加到初始脂质混合物中还是在脂质体形成后插入的影响。我们相信,对控制不均匀程度的因素的深入了解为生产更均匀的脂质体药物递送系统提供了可能性,这可能会提高它们的治疗效果。

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