丝裂吞噬增强型纳米粒子工程线粒体可恢复线粒体池的平衡,从而缓解肺纤维化。

IF 15.8 1区 材料科学 Q1 CHEMISTRY, MULTIDISCIPLINARY
ACS Nano Pub Date : 2024-11-15 DOI:10.1021/acsnano.4c10328
Yi Wang, Li-Fan Hu, Na-Hui Liu, Jing-Song Yang, Lei Xing, Jee-Heon Jeong, Ling Li, Hu-Lin Jiang
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引用次数: 0

摘要

肺纤维化(PF)是一种间质性肺病,与线粒体池平衡的破坏密切相关。线粒体转移是一项新兴技术,可通过外源线粒体输送增加功能线粒体;然而,在线粒体转移过程中,功能障碍线粒体的持续存在阻碍了线粒体转移的治疗效果,这归因于线粒体吞噬功能受损。在此,我们报道了由有丝分裂强化纳米粒子(Mito-MEN)介导的线粒体工程,它促进了功能性线粒体和功能障碍线粒体的同步调控,从而治疗PF。通过包裹Parkin mRNA制备了丝裂吞噬增强纳米颗粒(MENs),静电相互作用有利于MENs锚定分离的健康线粒体以构建Mito-MEN。Mito-MEN通过提高线粒体输送效率增加了功能性外源线粒体的负荷,并促进了功能障碍内源线粒体的有丝分裂。在博来霉素(BLM)诱导的PF小鼠模型中,Mito-MEN修复了线粒体功能,有效缓解了PF相关表型。这项研究为同步调整线粒体池平衡提供了有力工具,并为泛线粒体疾病疗法提供了一种转化方法。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

Mitophagy-Enhanced Nanoparticle-Engineered Mitochondria Restore Homeostasis of Mitochondrial Pool for Alleviating Pulmonary Fibrosis.

Mitophagy-Enhanced Nanoparticle-Engineered Mitochondria Restore Homeostasis of Mitochondrial Pool for Alleviating Pulmonary Fibrosis.

Pulmonary fibrosis (PF) is an interstitial lung disease tightly associated with the disruption of mitochondrial pool homeostasis, a delicate balance influenced by functional and dysfunctional mitochondria within lung cells. Mitochondrial transfer is an emerging technology to increase functional mitochondria via exogenous mitochondrial delivery; however, the therapeutic effect on mitochondrial transfer is hampered during the PF process by the persistence of dysfunctional mitochondria, which is attributed to impaired mitophagy. Herein, we reported engineering mitochondria mediated by mitophagy-enhanced nanoparticle (Mito-MEN), which promoted synchronal regulation of functional and dysfunctional mitochondria for treating PF. Mitophagy-enhanced nanoparticles (MENs) were fabricated through the encapsulation of Parkin mRNA, and the electrostatic interaction favored MENs to anchor isolated healthy mitochondria for the construction of Mito-MEN. Mito-MEN increased the load of functional exogenous mitochondria by enhancing mitochondrial delivery efficiency and promoted mitophagy of dysfunctional endogenous mitochondria. In a bleomycin (BLM)-induced PF mouse model, Mito-MEN repaired mitochondrial function and efficiently relieved PF-related phenotypes. This study provides a powerful tool for synchronal adjustment of mitochondrial pool homeostasis and offers a translational approach for pan-mitochondrial disease therapies.

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来源期刊
ACS Nano
ACS Nano 工程技术-材料科学:综合
CiteScore
26.00
自引率
4.10%
发文量
1627
审稿时长
1.7 months
期刊介绍: ACS Nano, published monthly, serves as an international forum for comprehensive articles on nanoscience and nanotechnology research at the intersections of chemistry, biology, materials science, physics, and engineering. The journal fosters communication among scientists in these communities, facilitating collaboration, new research opportunities, and advancements through discoveries. ACS Nano covers synthesis, assembly, characterization, theory, and simulation of nanostructures, nanobiotechnology, nanofabrication, methods and tools for nanoscience and nanotechnology, and self- and directed-assembly. Alongside original research articles, it offers thorough reviews, perspectives on cutting-edge research, and discussions envisioning the future of nanoscience and nanotechnology.
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