心脏毒性
材料科学
内质网
毒性
氧化应激
纳米颗粒
DNA损伤
药理学
纳米技术
医学
细胞生物学
内科学
癌症研究
生物物理学
生物
生物化学
DNA
作者
Rendong He,Xuefeng Ding,Tingjun Zhang,Linqiang Mei,Shuang Zhu,Chengyan Wang,You Liao,Dongmei Wang,Hao Wang,Junsong Guo,Xiaolan Guo,Yan Xing,Zhanjun Gu,Houxiang Hu
标识
DOI:10.1080/17435390.2023.2255269
摘要
Lead halide perovskites (LHPs) are outstanding candidates for next-generation optoelectronic materials, with considerable prospects of use and commercial value. However, knowledge about their toxicity is scarce, which may limit their commercialization. Here, for the first time, we studied the cardiotoxicity and molecular mechanisms of representative CsPbBr3 nanoparticles in LHPs. After their intranasal administration to Institute of Cancer Research (ICR) mice, using advanced synchrotron radiation, mass spectrometry, and ultrasound imaging, we revealed that CsPbBr3 nanoparticles can severely affect cardiac systolic function by accumulating in the myocardial tissue. RNA sequencing and Western blotting demonstrated that CsPbBr3 nanoparticles induced excessive oxidative stress in cardiomyocytes, thereby provoking endoplasmic reticulum stress, disturbing calcium homeostasis, and ultimately leading to apoptosis. Our findings highlight the cardiotoxic effects of LHPs and provide crucial toxicological data for the product.
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