心脏毒性
炎症
阿霉素
癌症研究
蒽环类
材料科学
活性氧
免疫系统
药理学
化学
医学
免疫学
内科学
生物化学
毒性
癌症
化疗
乳腺癌
作者
Zhinan Wang,Xi Liu,Xiaowei Zhu,Shidong Hu,Kun Zhang,Xiao‐Ting Li,Bin’en Nie,Ying‐Shi Sun
出处
期刊:Small
[Wiley]
日期:2025-10-22
标识
DOI:10.1002/smll.202508419
摘要
Abstract Doxorubicin (DOX), a widely used anthracycline chemotherapeutic, is clinically limited by cumulative and dose‐dependent cardiotoxicity. Oxidative stress and inflammation are central pathogenic mechanisms of DOX‐induced cardiomyopathy (DIC), characterized by extensive innate immune cells infiltration into the injured myocardium. The immune landscape of DIC mouse models is systematically characterized, identifying macrophages as the predominant immune subset. Based on this, a hybrid nanozyme (PB@CeO 2 NPs) is developed, comprising Prussian blue nanoparticles (PB NPs) and cerium oxide nanoparticles (CeO 2 NPs). The PB NPs core provides magnetic resonance imaging (MRI) contrast, while CeO 2 NPs surface modification enhances immune cell uptake, promotes retention in inflamed cardiac tissue, and augments reactive oxygen species (ROS) scavenging and anti‐inflammatory efficacy. In vitro experiments demonstrate that PB@CeO 2 NPs alleviate mitochondrial damage, inhibit apoptosis, and induce macrophage M2 polarization. In vivo studies show that PB@CeO 2 NPs facilitate myocardial accumulation, reduce cardiac inflammation and fibrosis, and improve cardiac function. By integrating the antioxidative and anti‐inflammatory effects of PB@CeO 2 NPs with inflammation‐mediated immune cell retention in injured myocardium, this study presents a promising nanotherapeutic platform for targeted and precise intervention in anthracycline‐induced cardiotoxicity.
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