诱导型环氧化酶表达介导缺氧/复氧诱导的肺血管收缩,在大鼠中被环氧化酶抑制剂减弱。
Inducible cyclooxygenase expression mediating hypoxia/reoxygenation-induced pulmonary vasoconstriction is attenuated by a cyclooxygenase inhibitor in rats.
作者信息
Su C L, Yuan D W, Chiang L L, Lee H L, Chen K H, Wang D
机构信息
Department of Chemistry, Graduate Institute of Basic Medicine, Fu Jen Catholic University, New Taipei City, Taiwan.
出版信息
Transplant Proc. 2012 May;44(4):929-32. doi: 10.1016/j.transproceed.2012.03.005.
OBJECTIVE
Hypoxic pulmonary vasoconstriction (HPV) is a well known phenomenon to temporarily offset a ventilation-perfusion mismatch. Sustained HPV may lead to pulmonary hypertension. In this protocol, we studied the relationships between the HPV response and inducible cyclooxygenase II (COX II) activation after hypoxia-reoxygenation (H-R) challenge in an isolated perfused lung model.
METHODS
An in situ isolated perfused rat lung model underwent inaction of hypoxia by ventilation with 5% CO(2)-95% N(2) for 10 minutes instead of 5% CO(2)-95% air; they were then reoxygenated with 5% CO(2)-95% air. We measured pulmonary arterial pressure (PAP) changes before, during, and after H-R challenge. We also estimated changes in blood concentrations of hydroxyl radicals, nitric oxide (NO) and thromboxane B(2) (TxB(2)) before and after H-R as well as mRNA expressions of COX II in lung tissue thereafter. A COX II inhibitor, celecoxib (10 mg/kg), was administered between 2 consecutive challenges.
RESULTS
Hypoxia induced pulmonary vasoconstriction by increasing PAP (4.1 ± 0.8 mm Hg). Consecutive hypoxic challenges did not show tachyphylaxis (P > .05). H-R of lung tissues induced significant increases in blood concentrations of hydroxyl radicals (48.5 ± 7.6 vs 75.8 ± 11.5 mmol/L; P < .01), NO (54.3 ± 12.3 vs 77.7 ± 15.7 pmol; P < .05), and TxB(2) (42.3 ± 6.9 vs 58.7 ± 8.6 pg/mL; P < .05). Lung tissue H-R also significantly increased COX II mRNA expression compared with sham tissues (1 ± 0 vs 4.0 ± 2.8; P < .001). The COX II inhibitor celecoxib significantly attenuated HPV responses (P < .05) and attenuated the elevated blood concentrations of TxB(2) (P < .05), hydroxyl radicals (P < .01), nitric oxide (P < .05), and COX II mRNA expression (P < .05) after H-R challenge.
CONCLUSIONS
Lung tissue H-R induced significant increases blood concentrations of inflammatory mediators and tissue mRNA expression of COX related to elevation of HPV responses. COX II inhibitor celecoxib attenuated the HPV responses by reducing TxB(2) release.
目的
低氧性肺血管收缩(HPV)是一种众所周知的现象,可暂时抵消通气-灌注不匹配。持续性HPV可能导致肺动脉高压。在本实验方案中,我们在离体灌注肺模型中研究了低氧复氧(H-R)刺激后HPV反应与诱导型环氧化酶II(COX II)激活之间的关系。
方法
采用原位离体灌注大鼠肺模型,用5%二氧化碳-95%氮气通气10分钟而非5%二氧化碳-95%空气进行低氧处理;然后用5%二氧化碳-95%空气复氧。我们测量了H-R刺激前、期间和之后的肺动脉压(PAP)变化。我们还估计了H-R前后血液中羟自由基、一氧化氮(NO)和血栓素B2(TxB2)浓度的变化以及此后肺组织中COX II的mRNA表达。在连续两次刺激之间给予COX II抑制剂塞来昔布(10 mg/kg)。
结果
低氧通过增加PAP(4.1±0.8 mmHg)诱导肺血管收缩。连续的低氧刺激未显示快速耐受(P>.05)。肺组织的H-R导致血液中羟自由基(48.5±7.6对75.8±11.5 mmol/L;P<.01)、NO(54.3±12.3对77.7±15.7 pmol;P<.05)和TxB2(42.3±6.9对58.7±8.6 pg/mL;P<.05)浓度显著增加。与假手术组相比,肺组织H-R也显著增加了COX II mRNA表达(1±0对4.0±2.8;P<.001)。COX II抑制剂塞来昔布显著减弱了HPV反应(P<.05),并减弱了H-R刺激后血液中TxB2(P<.05)、羟自由基(P<.01)、一氧化氮(P<.05)浓度的升高以及COX II mRNA表达(P<.05)。
结论
肺组织H-R导致与HPV反应增强相关的炎症介质血液浓度显著增加以及COX的组织mRNA表达增加。COX II抑制剂塞来昔布通过减少TxB2释放减弱了HPV反应。
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