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以乙醇为降解产物的缩醛化葡聚糖聚合物和微球的合成与表征。

Synthesis and characterization of acetalated dextran polymer and microparticles with ethanol as a degradation product.

机构信息

William G. Lowrie Department of Chemical and Biomolecular Engineering, College of Engineering, The Ohio State University, Columbus, Ohio 43210, United States.

出版信息

ACS Appl Mater Interfaces. 2012 Aug;4(8):4149-55. doi: 10.1021/am3008888. Epub 2012 Aug 2.

Abstract

In the field of drug delivery, pH-sensitive polymeric microparticles can be used to release therapeutic payloads slowly in extracellular conditions (pH 7.4) and faster in more acidic areas in vivo, such as sites of inflammation, tumors, or intracellular conditions. Our group currently uses and is further developing the pH-sensitive polymer acetalated dextran (Ac-DEX), which is a biodegradable polymer with highly tunable degradation kinetics. Ac-DEX has displayed enhanced delivery of vaccine and drug components to immune and other cells, making it an extremely desirable polymer for immune applications. Currently, one of the degradation products of Ac-DEX is methanol, which may cause toxicity issues if applied at high concentrations with repeated doses. Therefore, in this manuscript we report the first synthesis and characterization of an Ac-DEX analog which, instead of a methanol degradation product, has a much safer ethanol degradation product. We abbreviate this ethoxy acetal derivatized acetalated dextran polymer as Ace-DEX, with the 'e' to indicate an ethanol degradation product. Like Ac-DEX, Ace-DEX microparticles have tunable degradation rates at pH 5 (intracellular). These rates range from hours to several days and are controlled simply by reaction time. Ace-DEX microparticles also show minimal cytotoxicity compared to commonly used poly(lactic-co-glycolic acid) (PLGA) microparticles when incubated with macrophages. This study aims to enhance the biocompatibility of acetalated dextran-type polymers to allow their use in high volume clinical applications such as multiple dosing and tissue engineering.

摘要

在药物传递领域,pH 敏感型聚合物微球可用于在细胞外环境(pH7.4)中缓慢释放治疗性有效载荷,而在体内更酸性的区域(如炎症、肿瘤或细胞内部位)更快地释放。我们的团队目前正在使用并进一步开发 pH 敏感聚合物乙酰化葡聚糖(Ac-DEX),它是一种具有高度可调节降解动力学的可生物降解聚合物。Ac-DEX 已显示出对免疫和其他细胞的疫苗和药物成分的传递增强作用,使其成为免疫应用的理想聚合物。目前,Ac-DEX 的一种降解产物是甲醇,如果以高浓度重复使用,可能会引起毒性问题。因此,在本文中,我们报告了首例 Ac-DEX 类似物的合成和表征,该类似物的降解产物不是甲醇,而是更安全的乙醇。我们将这种乙氧基乙缩醛衍生的乙酰化葡聚糖聚合物简称为 Ace-DEX,其中“e”表示乙醇降解产物。与 Ac-DEX 一样,Ace-DEX 微球在 pH5(细胞内)下具有可调节的降解速率。这些速率范围从几小时到几天不等,并且可以通过反应时间简单控制。与常用的聚(乳酸-共-乙醇酸)(PLGA)微球相比,Ace-DEX 微球在与巨噬细胞孵育时表现出最小的细胞毒性。本研究旨在提高乙酰化葡聚糖类聚合物的生物相容性,使其能够在高剂量临床应用中使用,如多次给药和组织工程。

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