Nucleation-Inhibited Emulsion Interfacial Assembled Polydopamine Microvesicles as Artificial Antigen-Presenting Cells

IF 13 2区 材料科学 Q1 CHEMISTRY, MULTIDISCIPLINARY
Small Pub Date : 2024-04-09 DOI:10.1002/smll.202400714
Lingkai Dong, Minchao Liu, Meng Fang, Qianqian Lu, Xingjin Li, Yanming Ma, Tiancong Zhao
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引用次数: 0

Abstract

Albeit microemulsion systems have emerged as efficient platforms for fabricating tunable nano/microstructures, lack of understanding on the emulsion-interfacial assembly hindered the control of fabrication. Herein, a nucleation-inhibited microemulsion interfacial assembly method is proposed, which deviates from conventional interfacial nucleation approaches, for the synthesis of polydopamine microvesicles (PDA MVs). These PDA MVs exhibit an approximate diameter of 1 µm, showcasing a pliable structure reminiscent of cellular morphology. Through modifications of antibodies on the surface of PDA MVs, their capacity as artificial antigen presentation cells is evaluated. In comparison to solid nanoparticles, PDA MVs with cell-like structures show enhanced T-cell activation, resulting in a 1.5-fold increase in CD25 expression after 1 day and a threefold surge in PD-1 positivity after 7 days. In summary, the research elucidates the influence of nucleation and interfacial assembly in microemulsion polymerization systems, providing a direct synthesis method for MVs and substantiating their effectiveness as artificial antigen-presenting cells.

抑制成核的乳液界面组装聚多巴胺微囊作为人工抗原递呈细胞
尽管微乳液系统已成为制造可调纳米/微结构的高效平台,但对乳液界面组装缺乏了解阻碍了对制造的控制。本文提出了一种有别于传统界面成核方法的成核抑制微乳液界面组装方法,用于合成聚多巴胺微囊(PDA MVs)。这些聚多巴胺微囊的直径约为 1 微米,具有类似细胞形态的柔韧结构。通过对 PDA 微囊表面的抗体进行修饰,对其作为人工抗原递呈细胞的能力进行了评估。与固体纳米粒子相比,具有细胞样结构的 PDA MVs 能增强 T 细胞的活化,1 天后 CD25 表达增加 1.5 倍,7 天后 PD-1 阳性激增 3 倍。总之,这项研究阐明了微乳液聚合系统中成核和界面组装的影响,提供了一种直接合成 MVs 的方法,并证实了它们作为人工抗原递呈细胞的有效性。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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来源期刊
Small
Small 工程技术-材料科学:综合
CiteScore
17.70
自引率
3.80%
发文量
1830
审稿时长
2.1 months
期刊介绍: Small serves as an exceptional platform for both experimental and theoretical studies in fundamental and applied interdisciplinary research at the nano- and microscale. The journal offers a compelling mix of peer-reviewed Research Articles, Reviews, Perspectives, and Comments. With a remarkable 2022 Journal Impact Factor of 13.3 (Journal Citation Reports from Clarivate Analytics, 2023), Small remains among the top multidisciplinary journals, covering a wide range of topics at the interface of materials science, chemistry, physics, engineering, medicine, and biology. Small's readership includes biochemists, biologists, biomedical scientists, chemists, engineers, information technologists, materials scientists, physicists, and theoreticians alike.
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