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Interleukin-2 Functionalized Nanocapsules for T Cell-Based lmmunotherapy

机译:白细胞介素2功能化的纳米胶囊,用于基于T细胞的免疫治疗

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摘要

A major demand on immunotherapy is the direct interference with specific immune cells in vivo. In contrast to antibody engineered nanoparticles to control dendritic cells function, targeting of T cells for biomedical applications still remains an obstacle as they disclose reduced endocytic activities. Here, by coupling the cytokine interleukin-2 (IL-2) to the surface of hydroxyethyl starch nanocapsules, we demonstrated a direct and specifc T cell targeting in vitro and in vivo by IL-2 receptor-mediated internalization. For this purpose, defined amounts of azide-functionalized IL-2 were linked to alkyne-functionalized hydroxyethyl starch nanocapsules via copper-free click reactions. In combination with validated quantification of the surface-linked IL-2 with anthracen azide, this method allowed for engineering IL-2-functionalized nanocapsules for an efficient targeting of human and murine T cell populations with various IL-2 receptor affinities. This nanocapsulemediated technique is a promising strategy for T cell-based immunotherapies and may be translated to other cytokinerelated targeting systems.
机译:对免疫疗法的主要需求是体内特异性免疫细胞的直接干扰。与抗体工程化的纳米颗粒控制树突状细胞的功能相反,针对T细胞进行生物医学应用的目标仍然是一个障碍,因为它们揭示了减少的内吞活性。在这里,通过将细胞因子白介素2(IL-2)偶联到羟乙基淀粉纳米胶囊的表面,我们证明了通过IL-2受体介导的内在作用在体外和体内靶向直接和特异性的T细胞。为此,通过无铜点击反应将确定量的叠氮化物官能化的IL-2与炔烃官能化的羟乙基淀粉纳米胶囊连接。与用蒽叠氮化物对表面连接的IL-2进行定量验证相结合,该方法可对IL-2官能化的纳米胶囊进行改造,从而有效靶向具有各种IL-2受体亲和力的人和鼠T细胞群体。这种纳米胶囊介导的技术是基于T细胞的免疫疗法的一种有前途的策略,并且可以翻译为其他细胞因子相关的靶向系统。

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