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将细胞外囊泡重新设计为智能纳米尺度治疗剂。

Re-Engineering Extracellular Vesicles as Smart Nanoscale Therapeutics.

机构信息

Department of Materials, Department of Bioengineering, and Institute for Biomedical Engineering, Imperial College London , London SW7 2AZ, United Kingdom.

出版信息

ACS Nano. 2017 Jan 24;11(1):69-83. doi: 10.1021/acsnano.6b07607. Epub 2017 Jan 9.

Abstract

In the past decade, extracellular vesicles (EVs) have emerged as a key cell-free strategy for the treatment of a range of pathologies, including cancer, myocardial infarction, and inflammatory diseases. Indeed, the field is rapidly transitioning from promising in vitro reports toward in vivo animal models and early clinical studies. These investigations exploit the high physicochemical stability and biocompatibility of EVs as well as their innate capacity to communicate with cells via signal transduction and membrane fusion. This review focuses on methods in which EVs can be chemically or biologically modified to broaden, alter, or enhance their therapeutic capability. We examine two broad strategies, which have been used to introduce a wide range of nanoparticles, reporter systems, targeting peptides, pharmaceutics, and functional RNA molecules. First, we explore how EVs can be modified by manipulating their parent cells, either through genetic or metabolic engineering or by introducing exogenous material that is subsequently incorporated into secreted EVs. Second, we consider how EVs can be directly functionalized using strategies such as hydrophobic insertion, covalent surface chemistry, and membrane permeabilization. We discuss the historical context of each specific technology, present prominent examples, and evaluate the complexities, potential pitfalls, and opportunities presented by different re-engineering strategies.

摘要

在过去的十年中,细胞外囊泡(EVs)作为一种治疗多种疾病(包括癌症、心肌梗死和炎症性疾病)的关键无细胞策略,已经崭露头角。事实上,该领域正迅速从有前景的体外报告转向体内动物模型和早期临床研究。这些研究利用 EVs 的高物理化学稳定性和生物相容性,以及它们通过信号转导和膜融合与细胞进行通讯的固有能力。本文重点介绍了可以通过化学或生物学方法修饰 EVs,以拓宽、改变或增强其治疗能力的方法。我们研究了两种广泛使用的策略,这些策略已被用于引入各种纳米颗粒、报告系统、靶向肽、药物和功能性 RNA 分子。首先,我们探讨了如何通过操纵其亲代细胞来修饰 EVs,这些方法包括遗传或代谢工程,或者引入随后被纳入分泌的 EVs 的外源性物质。其次,我们考虑了如何使用疏水插入、共价表面化学和膜通透性等策略直接对 EVs 进行功能化。我们讨论了每种特定技术的历史背景,介绍了突出的例子,并评估了不同再工程策略所带来的复杂性、潜在陷阱和机会。

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