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通过无铜点击化学对等离子体细胞外囊泡进行功能化的标准化方法,用于靶向药物传递策略。

Standardized Method to Functionalize Plasma-Extracellular Vesicles via Copper-Free Click Chemistry for Targeted Drug Delivery Strategies.

机构信息

Department of Experimental Medicine, University of Genova, Largo Rosanna Benzi 10, Genova 16132, Italy.

UO Molecular Pathology, IRCCS Ospedale Policlinico San Martino, Largo Rosanna Benzi 10, Genova 16132, Italy.

出版信息

ACS Appl Bio Mater. 2024 Feb 19;7(2):827-838. doi: 10.1021/acsabm.3c00822. Epub 2024 Jan 16.

DOI:10.1021/acsabm.3c00822
PMID:38227342
Abstract

Extracellular vesicles (EVs) have emerged as potential vehicles for targeted drug delivery and diagnostic applications. However, achieving consistent and reliable functionalization of EV membranes remains a challenge. Copper-catalyzed click chemistry, commonly used for EV surface modification, poses limitations due to cytotoxicity and interference with biological systems. To overcome these limitations, we developed a standardized method for functionalizing an EV membrane via copper-free click chemistry. EVs derived from plasma hold immense potential as diagnostic and therapeutic agents. However, the isolation and functionalization of EVs from such a complex biofluid represent considerable challenges. We compared three different EV isolation methods to obtain an EV suspension with an optimal purity/yield ratio, and we identified sucrose cushion ultracentrifugation (sUC) as the ideal protocol. We then optimized the reaction conditions to successfully functionalize the plasma-EV surface through a copper-free click chemistry strategy with a fluorescently labeled azide, used as a proof-of-principle molecule. Click-EVs maintained their identity, size, and, more importantly, capacity to be efficiently taken up by responder tumor cells. Moreover, once internalized, click EVs partially followed the endosomal recycling route. The optimized reaction conditions and characterization techniques presented in this study offer a foundation for future investigations and applications of functionalized EVs in drug delivery, diagnostics, and therapeutics.

摘要

细胞外囊泡 (EVs) 已成为靶向药物递送和诊断应用的潜在载体。然而,实现 EV 膜的一致且可靠的功能化仍然是一个挑战。铜催化的点击化学,常用于 EV 表面修饰,由于细胞毒性和对生物系统的干扰,存在局限性。为了克服这些限制,我们开发了一种通过无铜点击化学对 EV 膜进行功能化的标准化方法。源自血浆的 EV 具有作为诊断和治疗剂的巨大潜力。然而,从如此复杂的生物流体中分离和功能化 EV 代表着相当大的挑战。我们比较了三种不同的 EV 分离方法,以获得具有最佳纯度/产率比的 EV 悬浮液,并确定蔗糖垫超速离心 (sUC) 是理想的方案。然后,我们优化了反应条件,通过铜自由点击化学策略成功地在荧光标记的叠氮化物上对血浆-EV 表面进行功能化,该叠氮化物被用作原理验证分子。点击-EVs 保持了它们的身份、大小,更重要的是,能够被 responder 肿瘤细胞高效摄取的能力。此外,一旦被内化,点击 EV 就会部分遵循内体再循环途径。本研究中提出的优化反应条件和表征技术为功能化 EV 在药物递送、诊断和治疗中的未来研究和应用提供了基础。

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