Mitochondrial endogenous substance transport-inspired nanomaterials for mitochondria-targeted gene delivery

IF 15.2 1区 医学 Q1 PHARMACOLOGY & PHARMACY
Yi Wang , Jing-Song Yang , Min Zhao , Jia-Qi Chen , Hai-Xin Xie , Hao-Yuan Yu , Na-Hui Liu , Zi-Juan Yi , Hui-Lin Liang , Lei Xing , Hu-Lin Jiang
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Abstract

Mitochondrial genome (mtDNA) independent of nuclear gene is a set of double-stranded circular DNA that encodes 13 proteins, 2 ribosomal RNAs and 22 mitochondrial transfer RNAs, all of which play vital roles in functions as well as behaviors of mitochondria. Mutations in mtDNA result in various mitochondrial disorders without available cures. However, the manipulation of mtDNA via the mitochondria-targeted gene delivery faces formidable barriers, particularly owing to the mitochondrial double membrane. Given the fact that there are various transport channels on the mitochondrial membrane used to transfer a variety of endogenous substances to maintain the normal functions of mitochondria, mitochondrial endogenous substance transport-inspired nanomaterials have been proposed for mitochondria-targeted gene delivery. In this review, we summarize mitochondria-targeted gene delivery systems based on different mitochondrial endogenous substance transport pathways. These are categorized into mitochondrial steroid hormones import pathways-inspired nanomaterials, protein import pathways-inspired nanomaterials and other mitochondria-targeted gene delivery nanomaterials. We also review the applications and challenges involved in current mitochondrial gene editing systems. This review delves into the approaches of mitochondria-targeted gene delivery, providing details on the design of mitochondria-targeted delivery systems and the limitations regarding the various technologies. Despite the progress in this field is currently slow, the ongoing exploration of mitochondrial endogenous substance transport and mitochondrial biological phenomena may act as a crucial breakthrough in the targeted delivery of gene into mitochondria and even the manipulation of mtDNA.

Abstract Image

用于线粒体靶向基因递送的线粒体内源性物质转运纳米材料。
线粒体基因组(mtDNA)独立于核基因,是一组双链环状 DNA,编码 13 种蛋白质、2 种核糖体 RNA 和 22 种线粒体转运 RNA,所有这些都对线粒体的功能和行为起着至关重要的作用。mtDNA 基因突变会导致各种线粒体疾病,且无药可治。然而,通过线粒体靶向基因递送操纵 mtDNA 面临着巨大的障碍,特别是由于线粒体双膜的存在。鉴于线粒体膜上有各种转运通道,用于转运各种内源性物质,以维持线粒体的正常功能,人们提出了线粒体内源性物质转运启发的纳米材料,用于线粒体靶向基因递送。在本综述中,我们总结了基于不同线粒体内源性物质转运途径的线粒体靶向基因递送系统。这些系统分为线粒体类固醇激素导入途径启发的纳米材料、蛋白质导入途径启发的纳米材料和其他线粒体靶向基因递送纳米材料。我们还回顾了目前线粒体基因编辑系统的应用和面临的挑战。本综述深入探讨了线粒体靶向基因递送的方法,详细介绍了线粒体靶向递送系统的设计以及不同技术的局限性。尽管这一领域目前进展缓慢,但对线粒体内源性物质转运和线粒体生物现象的不断探索,可能会成为向线粒体靶向传递基因甚至操纵 mtDNA 的关键突破口。
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
CiteScore
28.10
自引率
5.00%
发文量
294
审稿时长
15.1 weeks
期刊介绍: The aim of the Journal is to provide a forum for the critical analysis of advanced drug and gene delivery systems and their applications in human and veterinary medicine. The Journal has a broad scope, covering the key issues for effective drug and gene delivery, from administration to site-specific delivery. In general, the Journal publishes review articles in a Theme Issue format. Each Theme Issue provides a comprehensive and critical examination of current and emerging research on the design and development of advanced drug and gene delivery systems and their application to experimental and clinical therapeutics. The goal is to illustrate the pivotal role of a multidisciplinary approach to modern drug delivery, encompassing the application of sound biological and physicochemical principles to the engineering of drug delivery systems to meet the therapeutic need at hand. Importantly the Editorial Team of ADDR asks that the authors effectively window the extensive volume of literature, pick the important contributions and explain their importance, produce a forward looking identification of the challenges facing the field and produce a Conclusions section with expert recommendations to address the issues.
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