巨噬细胞极化
微泡
外体
炎症
细胞生物学
线粒体
巨噬细胞
化学
癌症研究
生物
免疫学
体外
小RNA
生物化学
基因
作者
Li Fan,Li Yao,Zhelong Li,Zhuo Wan,Wenqi Sun,Shuo Qiu,Wei Zhang,Dan Xiao,Liqiang Song,Guodong Yang,Yi Zhang,Mengying Wei,Xuekang Yang
标识
DOI:10.1002/advs.202205692
摘要
Abstract Sepsis is one of the most common causes of death, which is closely related to the uncontrolled systemic inflammation. Dysregulation of M1 macrophage polarization is the primary contributor to serious inflammation. In this study, it is revealed that the murine homologue of circRNA SCAR (steatohepatitis‐associated circRNA ATP5B regulator), denoted as circRNA mSCAR hereafter, decreases in the macrophages of septic mice, which correlates with the excessive M1 polarization. To restore circRNA mSCAR in mitochondria, exosomes encapsulated with circRNA mSCAR are further electroporated with poly‐D‐lysine‐graft‐triphenylphosphine (TPP‐PDL), and thus TPP‐PDL facilitates the bound circRNA delivered into mitochondria when the exosomes engulf by the recipient cells. In in vivo septic mouse model and in vitro cell model, it is shown that the exosome‐based mitochondria delivery system delivers circRNA mSCAR into mitochondria preferentially in the macrophages, favoring macrophage polarization toward M2 subtype. Accordingly, the systemic inflammation is attenuated by exosome‐based mitochondrial delivery of circRNA mSCAR, together with alleviated mortality. Collectively, the results uncover the critical role of circRNA mSCAR in sepsis, and provide a promising approach to attenuate sepsis via exosome‐based mitochondrial delivery of circRNA mSCAR.
科研通智能强力驱动
Strongly Powered by AbleSci AI