OBJECTIVES: The main goal of this work was to get insight into the mechanism of cerulein-induced reactive oxygen species (ROS) formation and impact of c-Jun NH(2)-terminal kinase (JNK) on this process. METHODS: The study was performed on Wistar rats and on a cellular model of acute pancreatitis (AP) using AR42J cell line. RESULTS: First of all, we observed that during AP, the iron storage protein ferritin in the rat pancreas undergoes degradation accompanied by an increased formation of protein carbonyls. Pancreatic acinar AR42J cells stimulated by cerulein showed increased labile iron pool that was accompanied by a decrease in the cellular ferritin-L level and an increase in the ROS formation. The changes in the ferritin-L level were inversely correlated with the ROS formation. The cells expressing inactive JNK1 mutant were completely resistant to cerulein-induced ferritin degradation. CONCLUSIONS: Our data showed that cerulein-induced AP in rats and on cellular model is accompanied by JNK1-dependent ferritin degradation, increases labile iron pool and ROS formation.
OBJECTIVES: The main goal of this work was to get insight into the mechanism of cerulein-induced reactive oxygen species (ROS) formation and impact of c-Jun NH(2)-terminal kinase (JNK) on this process. METHODS: The study was performed on Wistar rats and on a cellular model of acute pancreatitis (AP) using AR42J cell line. RESULTS: First of all, we observed that during AP, the iron storage protein ferritin in the rat pancreas undergoes degradation accompanied by an increased formation of protein carbonyls. Pancreatic acinar AR42J cells stimulated by cerulein showed increased labile iron pool that was accompanied by a decrease in the cellular ferritin-L level and an increase in the ROS formation. The changes in the ferritin-L level were inversely correlated with the ROS formation. The cells expressing inactive JNK1 mutant were completely resistant to cerulein-induced ferritin degradation. CONCLUSIONS: Our data showed that cerulein-induced AP in rats and on cellular model is accompanied by JNK1-dependent ferritin degradation, increases labile iron pool and ROS formation.
Authors: Andrew H Nguyen; Irmina A Elliott; Nanping Wu; Cynthia Matsumura; Maria Vogelauer; Narsis Attar; Amanda Dann; Razmik Ghukasyan; Paul A Toste; Sanjeet G Patel; Jennifer L Williams; Luyi Li; David W Dawson; Caius Radu; Siavash K Kurdistani; Timothy R Donahue Journal: Oncotarget Date: 2017-03-21
Authors: Pedro Silva-Vaz; Ana Margarida Abrantes; Miguel Castelo-Branco; António Gouveia; Maria Filomena Botelho; José Guilherme Tralhão Journal: Int J Mol Sci Date: 2019-06-07 Impact factor: 5.923
Authors: Marcus Hollenbach; Sebastian Sonnenberg; Ines Sommerer; Jana Lorenz; Albrecht Hoffmeister Journal: PLoS One Date: 2021-01-25 Impact factor: 3.240
Authors: Bomi Lee; Hong Namkoong; Yan Yang; Huang Huang; David Heller; Gregory L Szot; Mark M Davis; Sohail Z Husain; Stephen J Pandol; Melena D Bellin; Aida Habtezion Journal: Gut Date: 2021-10-26 Impact factor: 31.793