Nanoscale engineered exosomes for dual delivery of Sirtuin3 and insulin to ignite mitochondrial recovery in myocardial ischemia-reperfusion

纳米级工程化外泌体可双重递送Sirtuin3和胰岛素,以启动心肌缺血再灌注损伤后的线粒体恢复。

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作者:Jiaxin Yang # ,Xinyi Yun # ,Weihan Zheng # ,Huihui Zhang ,Zi Yan ,Youyu Chen ,Wanting Xue ,Siqi Mi ,Ziyue Li ,Hanxiao Sun ,Guozhi Xiao ,Zhenning Dai ,Shiyu Li ,Wenhua Huang
期刊:Journal of Nanobiotechnology影响因子:10.600
时间:2025起止号:2025 Jun 13;23(1):439.
doi:10.1186/s12951-025-03474-z研究方向: 炎症/感染
疾病类型: 心肌炎

Abstract

in English, German Background: Acute myocardial infarction remains a leading cause of mortality, with ischemia-reperfusion (I/R) injury causing severe myocardial damage through mitochondrial dysfunction. While mesenchymal stem cell-derived exosomes (MSC-Exo) show therapeutic potential, their limited targeting and insufficient mitochondrial protection restrict clinical application. Results: We developed a novel engineered exosome platform (Exo-I-S) using an IRES-driven bicistronic plasmid to co-load Sirtuin3 (SIRT3) and GPI-Insulin, aiming to enhance targeting efficiency and mitochondrial protection. The platform was evaluated in both in vitro and in vivo models of myocardial I/R injury. In vitro, Exo-I-S achieved faster cellular uptake, improved mitochondrial function, and reduced oxidative stress in H9c2 cells. The platform activated PI3K/AKT signaling, enhanced Glut4 translocation, and improved mitochondrial respiratory capacity. In a rat I/R injury model, Exo-I-S significantly reduced infarction size, improved cardiac function, and enhanced glucose metabolism, with superior therapeutic outcomes compared to unmodified exosomes. Conclusions: The dual functionality of Exo-I-S, combining insulin-mediated targeting with SIRT3-driven mitochondrial protection, provides a promising strategy for I/R injury treatment. Future studies should focus on optimizing targeting specificity and developing sustained release mechanisms to enhance clinical applicability.

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