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

线粒体 线粒体DNA 生物 细胞生物学 基因传递 线粒体融合 粒线体疾病 线粒体内膜 内生 基因 遗传增强 遗传学 生物化学
作者
Yi Wang,Jingsong Yang,Min Zhao,Jiaqi Chen,Hai-Xin Xie,Hao‐Yuan Yu,Na-Hui Liu,Zi-Juan Yi,Huilin Liang,Lei Xing,Hu‐Lin Jiang
出处
期刊:Advanced Drug Delivery Reviews [Elsevier]
卷期号:211: 115355-115355 被引量:6
标识
DOI:10.1016/j.addr.2024.115355
摘要

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 summary 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 involving in current mitochondrial gene editing systems. This review delves into the approaches of mitochondria-targeted gene delivery, providing detail on the design of mitochondria-targeted delivery systems and limitations regarding the varying 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.
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