用于抗原特异性t细胞接合的树突状细胞膜包被纳米颗粒的研制。

IF 5.5 2区医学 Q2 MATERIALS SCIENCE, BIOMATERIALS

ACS Biomaterials Science & Engineering Pub Date : 2025-10-03 DOI:10.1021/acsbiomaterials.5c01234

Sao Puth, Shruti Sunil Jadhav, Ali Zareein, Jimmy Blauser-Wilson, Mina Mahmoudi, Ruben Rojas Betanzos, Bayonel Ventura, Andrea M Sprague-Getsy, Xiaoran Hu, James L Hougland, Yaoying Wu

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引用次数: 0

摘要

树突状细胞（DC）膜包被纳米颗粒（DCmPs）具有抗原特异性治疗的巨大潜力。DCmPs携带促进DC- t细胞相互作用的关键DC膜蛋白，如主要组织相容性复合体（MHC）、共刺激CD80/86和粘附分子ICAM-1。然而，我们目前对涂层工艺和最终产品组成的影响的了解非常有限，这极大地阻碍了基于dcp的治疗的发展。本文利用DC2.4细胞膜蛋白和聚乳酸-羟基乙酸（PLGA）纳米颗粒，对超声、挤压和新开发的复合涂层方法（超声涂层后挤压工艺）制备的DCmPs的组成和功能进行了全面表征和比较。复合涂层方法获得了相对较高的蛋白质涂层水平，并且相对于超声和挤压，对DCmPs的直径和均匀性有更好的控制。我们还开发了一种表征策略，利用DCmPs和DC2.4细胞之间的同型相互作用，并确定约80%的PLGA颗粒被膜蛋白包裹，三种涂层过程后的最终产品中未结合的蛋白质和未包裹的颗粒相似。由于DC2.4细胞主要表达MHC I类分子，DCmPs与同源的B3Z CD8+ T细胞的结合优于DOBW CD4+ T细胞，证实DCmPs以抗原特异性的方式与T细胞结合。此外，我们证明DCmPs可以在体外激活B3Z CD8+ T细胞，类似于DC2.4细胞。这些发现表明了一种新的涂层方法，可以改善膜包覆颗粒的尺寸控制，并为详细分析包覆颗粒的组成提供了一种表征策略，这对DCmPs和其他膜包覆颗粒技术的治疗发展具有重要而广泛的意义。

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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Development of Dendritic Cell Membrane-Coated Nanoparticles for Antigen-Specific T-Cell Engagement.

Dendritic cell (DC) membrane-coated nanoparticles (DCmPs) hold significant potential for antigen-specific therapies. DCmPs carry key DC membrane proteins that facilitate DC-T cell interaction, such as the major histocompatibility complex (MHC), costimulatory CD80/86, and adhesive molecules ICAM-1. However, our current understanding of the impact of the coating processes and the composition of the final products is very limited, significantly hindering the development of DCmP-based therapy. Here, using DC2.4 cell membrane proteins and poly(lactic-co-glycolic acid) (PLGA) nanoparticles, we comprehensively characterized and compared the compositions and functions of DCmPs produced using sonication, extrusion, and a newly developed combined coating approach (sonication coating followed by extrusion process). The combined coating approach achieved a relatively high level of protein coating and exerted superior control over the diameter and uniformity of DCmPs relative to sonication and extrusion. We also developed a characterization strategy by leveraging the homotypic interactions between DCmPs and DC2.4 cells and determined that about 80% of PLGA particles are coated with membrane proteins, and both unbound proteins and uncoated particles are similarly present in the final products after the three coating processes. Because DC2.4 cells predominantly express MHC class I molecules, DCmPs showed preferential binding to cognate B3Z CD8+ T cells over DOBW CD4+ T cells, confirming that DCmPs bind to T cells in an antigen-specific fashion. Furthermore, we demonstrated that DCmPs can activate B3Z CD8+ T cells in vitro, similar to DC2.4 cells. These findings demonstrate a new coating approach that potentially improves size control over membrane-coated particles and a characterization strategy for detailed analysis of coated particle composition, which have important and broad implications for the therapeutic development of DCmPs and other membrane-coated particle technology.

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来源期刊

ACS Biomaterials Science & Engineering Materials Science-Biomaterials

CiteScore

10.30

自引率

3.40%

发文量

413

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