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首页> 外文期刊>Frontiers in Immunology >Activation of Human Complement System by Dextran-Coated Iron Oxide Nanoparticles Is Not Affected by Dextran/Fe Ratio, Hydroxyl Modifications, and Crosslinking
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Activation of Human Complement System by Dextran-Coated Iron Oxide Nanoparticles Is Not Affected by Dextran/Fe Ratio, Hydroxyl Modifications, and Crosslinking

机译:右旋糖酐/铁比,羟基修饰和交联不会影响右旋糖酐涂覆的氧化铁纳米粒子对人体补体系统的激活

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摘要

While having tremendous potential as therapeutic and imaging tools, the clinical use of engineered nanoparticles has been associated with serious safety concerns. Activation of the complement cascade and the release of proinflammatory factors C3a and C5a may contribute to infusion-related reactions, whereas opsonization with C3 fragments promotes rapid recognition and clearance of nanomaterials by mononuclear phagocytes. We used dextran-coated superparamagnetic iron oxide nanoparticles (SPIO), which are potent activators of the complement system, to study the role of nanoparticle surface chemistry in inciting complement in human serum. Using complement inhibitors and measuring levels of fluid phase markers (sC5b-9, C5a, and Bb), we found that the majority of human complement activation by SPIO is through the alternative pathways (AP). SPIO prepared with high dextran/iron ratio showed some complement activation via calcium-sensitive pathways, but the AP was responsible for the bulk of complement activation and amplification. Activation via the AP required properdin, the positive regulator of the alternative C3bBb convertase. Modification of sugar alcohols of dextran with alkylating, acylating, or crosslinking agents did not overcome complement activation and C3 opsonization. These data demonstrate that human complement activation is independent of dextran modification of SPIO and suggest a crucial role of the AP in immune recognition of nano-assemblies in human serum.
机译:尽管作为治疗和成像工具具有巨大潜力,但工程化纳米颗粒的临床使用已引起严重的安全隐患。补体级联的激活和促炎因子C3a和C5a的释放可能与输注相关的反应有关,而C3片段的调理作用可促进单核吞噬细胞对纳米材料的快速识别和清除。我们使用葡聚糖包被的超顺磁性氧化铁纳米颗粒(SPIO)作为补体系统的有效活化剂,来研究纳米颗粒表面化学在刺激人血清中补体中的作用。使用补体抑制剂并测量液相标记物(sC5b-9,C5a和Bb)的水平,我们发现SPIO激活的大多数人类补体都是通过替代途径(AP)。高葡聚糖/铁比的SPIO通过钙敏感途径表现出一些补体激活,但AP负责大部分补体激活和扩增。通过AP激活需要备解素,备择C3bBb转化酶的正调节剂。用烷基化,酰化或交联剂对葡聚糖糖醇的改性不能克服补体活化和C3调理作用。这些数据表明,人补体的激活与SPIO的右旋糖酐修饰无关,并暗示了AP在人血清中纳米组件的免疫识别中的关键作用。

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