%0 Journal Article %T Hydrogen gas inhalation protects against cigarette smokeinduced COPD development in mice %A Lu, Wenju %A Li, Defu %A Hu, Jieying %A Mei, Huijun %A Shu, Jiaze %A Long, Zhen %A Yuan, Liang %A Li, Difei %A Guan, Ruijuan %A Li, Yuanyuan %A Xu, Jingyi %A Wang, Tao %A Yao, Hongwei %A Zhong, Nanshan %A Zheng, Zeguang %J Journal of Thoracic Disease %D 2018 %B 2018 %9 %! Hydrogen gas inhalation protects against cigarette smokeinduced COPD development in mice %K %X Background: Chronic obstructive pulmonary disease (COPD) is a chronic lung disease with limited treatment options. Hydrogen (H 2 ) has been shown to be anti-oxidative and anti-inflammatory. This study aimed to evaluate the beneficial effects of H 2 inhalation on COPD development in mice. Methods: A COPD mouse model was established in male C57BL mice by cigarette smoke (CS) exposure. The H 2 intervention was administered by atomisation inhalation. Lung functions were assessed by using Buxco lung function measurement system. The inflammatory cells were counted and the levels of IL-6 and KC in BALF were assayed with ELISA. The lung tissue was subjected to H&E or PAS or Masson’s trichrome stain. Furthermore, 16HBE cells were used to evaluate the effects of H 2 on signaling change caused by hydrogen peroxide (H 2 O 2 ). H 2 O 2 was used to treat 16HBE cells with or without H 2 pretreatment. The IL-6 and IL-8 levels in cell culture medium were measured. The levels of phosphorylated ERK1/2 and nucleic NF-κB in lungs and 16HBE cells were determined. Results: H 2 ameliorated CS-induced lung function decline, emphysema, inflammatory cell infiltration, small-airway remodelling, goblet-cell hyperplasia in tracheal epithelium and activated ERK1/2 and NF-κB in mouse lung. In 16HBE airway cells, H 2 O 2 increased IL-6 and IL-8 secretion in conjunction with ERK1/2 and NF-κB activation. These changes were reduced by H 2 treatment. Conclusions: These findings demonstrated that H 2 inhalation could inhibit CS-induced COPD development in mice, which is associated with reduced ERK1/2 and NF-κB-dependent inflammatory responses. %U https://jtd.amegroups.org/article/view/22104 %V 10 %N 6 %P 3232-3243 %@ 2077-6624