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Cold stress increases reactive oxygen species formation via TRPA1 activation in A549 cells
Authors:Wenwu Sun  Zhonghua Wang  Jianping Cao  Haiyang Cui  Zhuang Ma
Institution:1.Department of Respiratory Medicine,General Hospital of Shenyang Military Area Command,Shenyang,China
Abstract:Reactive oxygen species (ROS) are responsible for lung damage during inhalation of cold air. However, the mechanism of the ROS production induced by cold stress in the lung is still unclear. In this work, we measured the changes of ROS and the cytosolic Ca2+ concentration (Ca2+]c) in A549 cell. We observed that cold stress (from 20 to 5 °C) exposure of A549 cell resulted in an increase of ROS and Ca2+]c, which was completely attenuated by removing Ca2+ from medium. Further experiments showed that cold-sensing transient receptor potential subfamily member 1 (TRPA1) agonist (allyl isothiocyanate, AITC) increased the production of ROS and the level of Ca2+]c in A549 cell. Moreover, HC-030031, a TRPA1 selective antagonist, significantly inhibited the enhanced ROS and Ca2+]c induced by AITC or cold stimulation, respectively. Taken together, these data demonstrated that TRPA1 activation played an important role in the enhanced production of ROS induced by cold stress in A549 cell.
Keywords:Cold stress  Reactive oxygen species  TRPA1  [Ca2+]c
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