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首页> 外文期刊>Journal of Materials Chemistry, B. materials for biology and medicine >Characterization of carbon-coated magnetic nanoparticles using clinical blood coagulation assays: effect of PEG-functionalization and comparison to silica nanoparticles
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Characterization of carbon-coated magnetic nanoparticles using clinical blood coagulation assays: effect of PEG-functionalization and comparison to silica nanoparticles

机译:使用临床血液凝固测定法表征碳包覆的磁性纳米粒子:PEG官能化的作用以及与二氧化硅纳米粒子的比较

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摘要

Intravascular application of magnetic nanocarriers is a critical step in the development of new therapeutic strategies, including magnetic drug targeting or hyperthermia. However, injection of particulate matter bears the intrinsic risk of contact activation of the blood coagulation cascade. In this work, we use point-of-care assays to study coagulation dynamics and clotting parameters in blood samples exposed to relevant concentrations of surface-functionalized carbon-coated iron carbide nanomagnets using unmodified nanomagnets and poly(ethylene)glycol-functionalized nanomagnets with different end-groups, including -OCH3, -NH2, -COOH, -IgG, and -ProteinA-protected-IgG HgG-ProtA). Silica nanoparticles with a comparable surface area are used as a reference material. For magnetic nanoparticles, we observe a decrease in clotting time by 25% compared to native blood at concentrations of 1 mg mL~(-1), independent of the surface functionalization, and only minor differences in receptor expression on platelets (GP-llb-llla, CD62, and CD63) relative to control samples were observed. Interestingly, the inter-subject variance of the clotting time is similar to the nanoparticle-induced effect in a single subject with average clotting time. Whilst the present study is based on in vitro assays and a small group of healthy blood donors, the comparison to broadly used silica nanoparticles, and the fact that experimental intergroup variability is comparable to the observed effects from the carbon-coated nanomagnets suggests continuing investigations on their potential clinical use.
机译:磁性纳米载体的血管内应用是新治疗策略(包括磁性药物靶向或热疗)发展中的关键步骤。然而,颗粒物质的注射具有引起凝血级联反应的接触的内在风险。在这项工作中,我们使用即时检测法研究暴露于相关浓度的表面功能化碳包覆的碳化铁纳米磁体的血样中的凝血动力学和凝血参数,使用未改性的纳米磁体和聚乙二醇官能化的纳米磁体,其中不同端基,包括-OCH3,-NH2,-COOH,-IgG和-ProteinA保护的IgG HgG-ProtA)。具有可比表面积的二氧化硅纳米颗粒用作参考材料。对于磁性纳米颗粒,我们观察到在浓度为1 mg mL〜(-1)的情况下,与天然血液相比,凝血时间减少了25%,而与表面功能无关,并且血小板受体表达的细微差异(GP-llb-观察到相对于对照样品的IIIa,CD62和CD63)。有趣的是,凝血时间的受试者间差异类似于具有平均凝血时间的单个受试者中纳米颗粒诱导的作用。尽管本研究基于体外试验和一小群健康的献血者,但与广泛使用的二氧化硅纳米颗粒的比较以及实验的组间变异性可与碳涂层纳米磁铁的观察结果相媲美这一事实表明,我们需要继续研究其潜在的临床用途。

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