Pioglitazone reduces angiotensin II-induced COX-2 expression through inhibition of ROS production and ET-1 transcription in vascular cells from spontaneously hypertensive rats

被引:22
作者
Perez-Giron, Jose V. [1 ]
Palacios, Roberto [1 ]
Martin, Angela [1 ]
Hernanz, Raquel [1 ]
Aguado, Andrea [2 ]
Martinez-Revelles, Sonia [2 ]
Barrus, Maria T. [1 ]
Salaices, Mercedes [2 ]
Alonso, Maria J. [1 ]
机构
[1] Univ Rey Juan Carlos, Dept Bioquim Fisiol & Genet Mol, Alcorcon 28922, Spain
[2] Univ Autonoma Madrid, Hosp Univ La Paz, Inst Invest, Dept Farmacol, Madrid, Spain
来源
AMERICAN JOURNAL OF PHYSIOLOGY-HEART AND CIRCULATORY PHYSIOLOGY | 2014年 / 306卷 / 11期
关键词
angiotensin II; endothelin-1; reactive oxygen species; cyclooxygenase-2; hypertension; peroxisome proliferator-activated receptor-gamma; ACTIVATED-RECEPTOR-GAMMA; SMOOTH-MUSCLE-CELLS; ENDOTHELIN-1; GENE-EXPRESSION; FACTOR-KAPPA-B; REGULATED KINASE PATHWAY; OXIDATIVE STRESS; NADPH OXIDASE; PPAR-GAMMA; CYCLOOXYGENASE-2; EXPRESSION; MOLECULAR-MECHANISMS;
D O I
10.1152/ajpheart.00924.2013
中图分类号
R5 [内科学];
学科分类号
1002 ; 100201 ;
摘要
Glitazones have anti-inflammatory properties by interfering with the transcription of proinflammatory genes, such as cyclooxygenase (COX)-2, and with ROS production, which are increased in hypertension. This study analyzed whether pioglitazone modulates COX-2 expression in hypertension by interfering with ROS and endothelin (ET)-1. In vivo, pioglitazone (2.5 mg.kg(-1).day(-1), 28 days) reduced the greater levels of COX-2, pre-pro-ET-1, and NADPH oxidase (NOX) expression and activity as well as O-2(-) production found in aortas from spontaneously hypertensive rats (SHRs). ANG II increased COX-2 and pre-pro-ET-1 levels more in cultured vascular smooth muscle cells from hypertensive rats compared with normotensive rats. The ETA receptor antagonist BQ-123 reduced ANG II-induced COX-2 expression in SHR cells. ANG II also increased NOX-1 expression, NOX activity, and superoxide production in SHR cells; the selective NOX-1 inhibitor ML-171 and catalase reduced ANG II-induced COX-2 and ET-1 transcription. ANG II also increased c-Jun transcription and phosphoJNK1/ 2, phospho-c-Jun, and p65 NF-kappa B subunit nuclear protein expression. SP-600125 and lactacystin, JNK and NF-kappa B inhibitors, respectively, reduced ANG II-induced ET-1, COX-2, and NOX-1 levels and NOX activity. Pioglitazone reduced the effects of ANG II on NOX activity, NOX-1, pre-pro-ET-1, COX-2, and c-Jun mRNA levels, JNK activation, and nuclear phospho-c-Jun and p65 expression. In conclusion, ROS production and ET-1 are involved in ANG II-induced COX-2 expression in SHRs, explaining the greater COX-2 expression observed in this strain. Furthermore, pioglitazone inhibits ANG II-induced COX-2 expression likely by interfering with NF-kappa B and activator protein-1 proinflammatory pathways and downregulating ROS production and ET-1 transcription, thus contributing to the anti-inflammatory properties of glitazones.
引用
收藏
页码:H1582 / H1593
页数:12
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