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基于聚多巴胺的血红蛋白颗粒表面修饰用于提高氧载体的稳定性。

Polydopamine-based surface modification of hemoglobin particles for stability enhancement of oxygen carriers.

机构信息

Institute of Health Service and Transfusion Medicine, Bejing 100850, China.

Institute of Health Service and Transfusion Medicine, Bejing 100850, China.

出版信息

J Colloid Interface Sci. 2020 Jul 1;571:326-336. doi: 10.1016/j.jcis.2020.03.046. Epub 2020 Mar 12.

DOI:10.1016/j.jcis.2020.03.046
PMID:32208203
Abstract

Templated assembly techniques have been extensively used to develop various types of hemoglobin (Hb) loaded particles with improved performance. However, several instability issues must still be solved, including Hb exposure, enhanced Hb auto-oxidation, and the relatively weak binding of Hb to cross-linkers. Herein, to meet the stability requirements for novel hemoglobin-based oxygen carriers (HBOCs), hemoglobin-polydopamine particles (Hb-PDA) were fabricated using a mild process that combines the co-precipitation of Hb and an inorganic template with the spontaneous adhesion of PDA. The Hb-PDA showed uniform size distribution, chemical integrity of both Hb and PDA, high biocompatibility, and robust oxygen delivery. Our results demonstrated that the use of polydopamine as a biocompatible coating material reduced Hb leakage from the particles under both static and flow conditions, thus mitigating the toxicity associated with free Hb and strengthening the stability of Hb particles. In addition, Hb-PDA reduced HUVEC (Human Umbilical Vein Cells) oxidative injury and scavenged 85% of the available hydroxyl radicals, exhibiting its potential to act as an antioxidant for encapsulated Hb. Hb-PDA therefore shows significant promise as a cell-like structurally and functionally stable HBOCs.

摘要

模板组装技术已被广泛用于开发各种类型的血红蛋白(Hb)负载颗粒,以提高其性能。然而,仍有几个不稳定性问题需要解决,包括 Hb 的暴露、增强的 Hb 自动氧化和 Hb 与交联剂的相对较弱结合。在此,为了满足新型血红蛋白类氧载体(HBOCs)的稳定性要求,使用一种温和的方法制备了血红蛋白-聚多巴胺颗粒(Hb-PDA),该方法结合了 Hb 和无机模板的共沉淀以及 PDA 的自发粘附。Hb-PDA 表现出均匀的粒径分布、Hb 和 PDA 的化学完整性、高生物相容性和强大的氧输送能力。我们的结果表明,使用聚多巴胺作为生物相容性涂层材料可以减少颗粒在静态和流动条件下 Hb 的泄漏,从而减轻游离 Hb 引起的毒性,并增强 Hb 颗粒的稳定性。此外,Hb-PDA 减轻了 HUVEC(人脐静脉细胞)的氧化损伤,并清除了 85%的可用羟基自由基,表明其有潜力作为包封 Hb 的抗氧化剂。因此,Hb-PDA 作为一种具有类似细胞结构和功能稳定的 HBOCs 具有很大的应用前景。

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