阿霉素
药理学
线粒体
细胞毒性
DNM1L型
细胞凋亡
氧化应激
生物
顺铂
细胞生物学
生物化学
线粒体分裂
体外
化疗
遗传学
作者
Jhong‐Kuei Chen,S. Ramesh,Md. Nazmul Islam,Marthandam Asokan Shibu,Chia‐Hua Kuo,Dennis Jine‐Yuan Hsieh,Shinn‐Zong Lin,Wei‐Wen Kuo,Chih‐Yang Huang,Tsung‐Jung Ho
摘要
Abstract The most effective drug, doxorubicin (DOX), is widely used worldwide for clinical application as an anticancer drug. DOX‐induced cytotoxicity is characterized by mitochondrial dysfunction. There is no alternative treatment against DOX‐induced cardiac damage despite intensive research in the present decades. Ohwia caudata has emerged as a potential herbal remedy that prevents from DOX‐induced cytotoxicity owing to its pharmacological action of sustaining mitochondrial dynamics by attenuating oxidative stress and inducing cellular longevity. However, its underlying mechanisms are unknown. The novel treatment provided here depends on new evidence from DOX‐treated H9c2 cells, which significantly enhanced insulin‐like growth factor (IGF) II receptor (IGF‐IIR) pathways that activated calcineurin and phosphorylated dynamin‐related protein 1 (p‐Drp1) at ser616 (p‐Drp1[ser616]); cells undergo apoptosis due to these factors, which translocate to mitochondria and disrupt their function and integrity, and in terms of herbal medicine treatment, which significantly blocked these phenomena. Thus, our findings indicate that maintaining integrity of mitochondria is an essential element in lowering DOX‐induced cytotoxicity, which further emphasizes that our herbal medicine can successfully block IGF‐IIR pathways and could potentially act as an alternative mechanism in terms of cardioprotective against doxorubicin.
科研通智能强力驱动
Strongly Powered by AbleSci AI