线粒体
失调家庭
粒线体疾病
医学
生物
化学
生物信息学
细胞生物学
线粒体DNA
生物化学
精神科
基因
作者
Yi Wang,Na-Hui Liu,Li‐Fan Hu,Jingsong Yang,Mengmeng Han,Tian‐Jiao Zhou,Lei Xing,Hu‐Lin Jiang
标识
DOI:10.1016/j.apsb.2024.08.007
摘要
an enhanced PARKIN-mediated mitophagy process. In a mouse model induced with a complex I inhibitor (rotenone, Rot), mNP-Mito enhanced the presence of healthy mitochondria and exhibited a sharp increase in complex I activity (76.5%) compared to the group exposed to Rot damage (29.5%), which greatly promoted the restoration of ATP generation and mitigation of ocular mitochondrial disease-related phenotypes. This study highlights the significance of nanoengineered mitochondria as a promising and feasible tool for the replacement of dysfunctional mitochondria and the repair of mitochondrial function in mitochondrial disease therapies.
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