| Literature DB >> 31557070 |
Muhammad Hasnat1,2, Ziqiao Yuan1, Aftab Ullah3, Muhammad Naveed4, Faisal Raza3, Mirza Muhammad Faran Ashraf Baig5, Asifullah Khan3, Dengqiu Xu1, Yuwen Su6,7, Linxin Sun1,8, Luyong Zhang1,9, Zhenzhou Jiang1,10.
Abstract
How triptolide is associated with mitochondrial dysfunction and apoptosis in connection with its hepatotoxicity remains unclear. The objective of our study was to find out the link between mitochondrial dynamics and cell death in triptolide induced hepatotoxicity. We treated L02 cells with 25 nM concentration of triptolide. The results demonstrated that triptolide treatment caused an increase in apoptotic cell death, mitochondrial depolarization, ROS overproduction, a decrease in ATP production, and mitochondrial fragmentation which in turn is associated with the activation of Drp1 fission protein. Triptolide treatment led to the translocation of Drp1 from the cytosol into outer mitochondrial membrane where it started mitochondrial fission. This fission event is coupled with the mitochondrial release of cytochrome c into the cytosol and subsequently caspase-3 activation. TEM analysis of rat liver tissues revealed the distortion of mitochondrial morphology in triptolide-treated group. Western blot analysis explained that disruption in mitochondrial morphology was attached with the recruitment of Drp1 to mitochondria, cytochrome c release, and caspase-3 activation. However, Mdivi-1 co-treatment inhibited the activation of Drp1 and caspase-3 and blocked the release of cytochrome c into the cytosol. In short, inhibiting Drp1 protein activation may provide a new potential target for curing Drp1-associated apoptosis in triptolide-induced hepatotoxicity.Entities:
Keywords: Drp1; Triptolide; apoptosis; hepatotoxicity; mitochondria
Year: 2019 PMID: 31557070 DOI: 10.1080/15376516.2019.1669247
Source DB: PubMed Journal: Toxicol Mech Methods ISSN: 1537-6516 Impact factor: 2.987