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Hyaluronan Nanoparticles Selectively Target Plaque-Associated Macrophages and Improve Plaque Stability in Atherosclerosis

机译:透明质酸纳米粒子选择性靶向斑块相关的巨噬细胞,并改善动脉粥样硬化斑块的稳定性。

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摘要

Hyaluronan is a biologically active polymer, which can be formulated into nanoparticles. In our study, we aimed to probe atherosclerosis-associated inflammation by using hyaluronan nanoparticles and to determine whether they can ameliorate atherosclerosis. Hyaluronan nanoparticles (HA-NPs) were prepared by reacting amine-functionalized oligomeric hyaluronan (HA) with cholanic ester and labeled with a fluorescent or radioactive label. HA-NPs were characterized in vitro by several advanced microscopy methods. The targeting properties and biodistribution of HA-NPs were studied in apoe(-/-) mice, which received either fluorescent or radiolabeled HA-NPs and were examined ex vivo by flow cytometry or nuclear techniques. Furthermore, three atherosclerotic rabbits received Zr-89-HA-NPs and were imaged by PET/MRI. The therapeutic effects of HA-NPs were studied in apoe(-/-) mice, which received weekly doses of 50 mg/kg HA-NPs during a 12-week high-fat diet feeding period. Hydrated HA-NPs were ca. 90 nm in diameter and displayed very stable morphology under hydrolysis conditions. Flow cytometry revealed a 6- to 40-fold higher uptake of Cy7-HA-NPs by aortic macrophages compared to normal tissue macrophages. Interestingly, both local and systemic HA-NP immune cell interactions significantly decreased over the disease progression. Zr-89-HA-NPs-induced radioactivity in atherosclerotic aortas was 30% higher than in wild-type controls. PET imaging of rabbits revealed 6-fold higher standardized uptake values compared to the muscle. The plaques of HA-NP-treated mice contained 30% fewer macrophages compared to control and free HA-treated group. In conclusion, we show favorable targeting properties of HA-NPs, which can be exploited for PET imaging of atherosclerosis-associated inflammation. Furthermore, we demonstrate the anti-inflammatory effects of HA-NPs in atherosclerosis
机译:透明质酸是一种生物活性聚合物,可以配制成纳米颗粒。在我们的研究中,我们旨在通过使用透明质酸纳米颗粒来探测与动脉粥样硬化相关的炎症,并确定它们是否可以改善动脉粥样硬化。通过使胺官能化的低聚乙酰透明质酸(HA)与胆酸酯反应并用荧光或放射性标记进行标记来制备透明质酸纳米颗粒(HA-NP)。 HA-NPs在体外通过几种先进的显微镜方法进行了表征。在载脂蛋白(-/-)小鼠中研究了HA-NP的靶向特性和生物分布,该小鼠接受了荧光或放射性标记的HA-NP,并通过流式细胞仪或核技术进行了离体检查。此外,三只动脉粥样硬化兔接受Zr-89-HA-NPs,并通过PET / MRI成像。在apoe(-/-)小鼠中研究了HA-NP的治疗效果,该小鼠在12周的高脂饮食喂养期间每周接受50 mg / kg的HA-NP剂量。水合的HA-NPs约为。直径为90 nm,在水解条件下显示出非常稳定的形态。流式细胞仪显示,与正常组织巨噬细胞相比,主动脉巨噬细胞对Cy7-HA-NPs的摄取高6至40倍。有趣的是,在疾病进展过程中,局部和全身性HA-NP免疫细胞相互作用均显着降低。 Zr-89-HA-NPs诱导的动脉粥样硬化主动脉放射性比野生型对照高30%。与肌肉相比,兔子的PET成像显示标准化摄取值高6倍。与对照组和游离HA治疗组相比,HA-NP治疗的小鼠的斑块包含的巨噬细胞减少了30%。总之,我们显示了HA-NPs的良好靶向特性,可用于与动脉粥样硬化相关的炎症的PET成像。此外,我们证明了HA-NP在动脉粥样硬化中的抗炎作用

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