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红细胞膜衍生纳米颗粒:其临床转化中的应用与关键挑战

Red blood cells membrane-derived nanoparticles: Applications and key challenges in their clinical translation.

作者信息

Malhotra Sahil, Dumoga Shweta, Singh Neetu

机构信息

Centre for Biomedical Engineering, Indian Institute of Technology Delhi, New Delhi, India.

Biomedical Engineering unit, All India Institute of Medical Sciences New Delhi, New Delhi, India.

出版信息

Wiley Interdiscip Rev Nanomed Nanobiotechnol. 2022 May;14(3):e1776. doi: 10.1002/wnan.1776. Epub 2022 Feb 1.

Abstract

Cellular membrane-derived nanoparticles, particularly of red blood cells (RBCs), represent an emerging class of drug delivery systems. The lack of nucleus and organelles in these cells makes them easy to process and empty out intracellular contents. The empty vesicle membranes can then be either used as a coating on nanoparticles or can be reassembled into a nanovesicle. Engineered RBCs membrane has unique ability to retain its lipid bilayer architecture with host's proteins during top-down approach, thus allowing it to form stable nanoformulations mimicking RBCs stealth properties. In addition, its core-shell structure allows loading of different drug molecules, and its surface chemistry can be manipulated by facile conjugation with ligands on the shell. The remarkable ability of RBCs membrane to fuse with membranes of other cells enables the formation of hybrid nanovesicles. In this review, we highlight the biomedical applications of such vesicles and discuss the potential challenges related to its clinical translation. Although nano-RBCs retain much of the host's proteins, which may give an edge over synthetic nanoparticles in terms of lower immunogenicity, its production at industrial level is more challenging. This review gives the critical analysis of barriers involved in the translation of RBCs-derived nanoparticles from preclinical to clinical level. This article is categorized under: Therapeutic Approaches and Drug Discovery > Emerging Technologies Biology-Inspired Nanomaterials > Lipid-Based Structures Toxicology and Regulatory Issues in Nanomedicine > Regulatory and Policy Issues in Nanomedicine.

摘要

细胞膜衍生的纳米颗粒,尤其是红细胞(RBC)来源的纳米颗粒,代表了一类新兴的药物递送系统。这些细胞缺乏细胞核和细胞器,使其易于处理并清空细胞内的内容物。然后,空的囊泡膜既可以用作纳米颗粒的涂层,也可以重新组装成纳米囊泡。在自上而下的方法中,工程化的红细胞膜具有在保留宿主蛋白质的同时保持其脂质双层结构的独特能力,从而使其能够形成模仿红细胞隐身特性的稳定纳米制剂。此外,其核壳结构允许加载不同的药物分子,并且其表面化学性质可以通过与壳上的配体进行简便的共轭来操纵。红细胞膜与其他细胞膜融合的卓越能力能够形成杂化纳米囊泡。在这篇综述中,我们重点介绍了此类囊泡的生物医学应用,并讨论了与其临床转化相关的潜在挑战。尽管纳米红细胞保留了许多宿主蛋白质,这在较低免疫原性方面可能比合成纳米颗粒具有优势,但其在工业规模上的生产更具挑战性。这篇综述对红细胞衍生的纳米颗粒从临床前到临床转化过程中涉及的障碍进行了批判性分析。本文分类如下:治疗方法与药物发现>新兴技术;受生物学启发的纳米材料>基于脂质的结构;纳米医学中的毒理学与监管问题>纳米医学中的监管与政策问题。

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