三羰基二氯钌（II）二聚体（CORM-2）释放的一氧化碳对实验性乙醇诱导的胃损伤的胃保护作用

Carbon Monoxide (CO) Released from Tricarbonyldichlororuthenium (II) Dimer (CORM-2) in Gastroprotection against Experimental Ethanol-Induced Gastric Damage.

作者信息

Magierowska Katarzyna, Magierowski Marcin, Hubalewska-Mazgaj Magdalena, Adamski Juliusz, Surmiak Marcin, Sliwowski Zbigniew, Kwiecien Slawomir, Brzozowski Tomasz

机构信息

Department of Physiology, Jagiellonian University Medical College, Cracow, Poland.

Department of Forensic Toxicology, Institute of Forensic Research, Cracow, Poland.

出版信息

PLoS One. 2015 Oct 13;10(10):e0140493. doi: 10.1371/journal.pone.0140493. eCollection 2015.

DOI:10.1371/journal.pone.0140493

PMID:26460608

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC4604159/

Abstract

The physiological gaseous molecule, carbon monoxide (CO) becomes a subject of extensive investigation due to its vasoactive activity throughout the body but its role in gastroprotection has been little investigated. We determined the mechanism of CO released from its donor tricarbonyldichlororuthenium (II) dimer (CORM-2) in protection of gastric mucosa against 75% ethanol-induced injury. Rats were pretreated with CORM-2 30 min prior to 75% ethanol with or without 1) non-selective (indomethacin) or selective cyclooxygenase (COX)-1 (SC-560) and COX-2 (celecoxib) inhibitors, 2) nitric oxide (NO) synthase inhibitor L-NNA, 3) ODQ, a soluble guanylyl cyclase (sGC) inhibitor, hemin, a heme oxygenase (HO)-1 inductor or zinc protoporphyrin IX (ZnPPIX), an inhibitor of HO-1 activity. The CO content in gastric mucosa and carboxyhemoglobin (COHb) level in blood was analyzed by gas chromatography. The gastric mucosal mRNA expression for HO-1, COX-1, COX-2, iNOS, IL-4, IL-1β was analyzed by real-time PCR while HO-1, HO-2 and Nrf2 protein expression was determined by Western Blot. Pretreatment with CORM-2 (0.5-10 mg/kg) dose-dependently attenuated ethanol-induced lesions and raised gastric blood flow (GBF) but large dose of 100 mg/kg was ineffective. CORM-2 (5 mg/kg and 50 mg/kg i.g.) significantly increased gastric mucosal CO content and whole blood COHb level. CORM-2-induced protection was reversed by indomethacin, SC-560 and significantly attenuated by celecoxib, ODQ and L-NNA. Hemin significantly reduced ethanol damage and raised GBF while ZnPPIX which exacerbated ethanol-induced injury inhibited CORM-2- and hemin-induced gastroprotection and the accompanying rise in GBF. CORM-2 significantly increased gastric mucosal HO-1 mRNA expression and decreased mRNA expression for iNOS, IL-1β, COX-1 and COX-2 but failed to affect HO-1 and Nrf2 protein expression decreased by ethanol. We conclude that CORM-2 released CO exerts gastroprotection against ethanol-induced gastric lesions involving an increase in gastric microcirculation mediated by sGC/cGMP, prostaglandins derived from COX-1, NO-NOS system and its anti-inflammatory properties.

摘要

生理性气体分子一氧化碳（CO）因其在全身的血管活性作用而成为广泛研究的对象，但其在胃保护中的作用却鲜有研究。我们确定了其供体二氯二羰基钌（II）二聚体（CORM-2）释放的CO在保护胃黏膜免受75%乙醇诱导损伤中的作用机制。在给予75%乙醇前30分钟，用CORM-2对大鼠进行预处理，同时给予或不给予以下物质：1）非选择性（吲哚美辛）或选择性环氧化酶（COX）-1（SC-560）和COX-2（塞来昔布）抑制剂；2）一氧化氮（NO）合酶抑制剂L-NNA；3）ODQ，一种可溶性鸟苷酸环化酶（sGC）抑制剂，血红素，一种血红素加氧酶（HO）-1诱导剂或锌原卟啉IX（ZnPPIX），一种HO-1活性抑制剂。通过气相色谱分析胃黏膜中的CO含量和血液中的碳氧血红蛋白（COHb）水平。通过实时PCR分析胃黏膜中HO-1、COX-1、COX-2、诱导型一氧化氮合酶（iNOS）、白细胞介素-4（IL-4）和白细胞介素-1β（IL-1β）的mRNA表达，同时通过蛋白质免疫印迹法测定HO-1、HO-2和核因子E2相关因子2（Nrf2）的蛋白表达。用CORM-2（0.5 - 10mg/kg）预处理可剂量依赖性地减轻乙醇诱导的损伤并增加胃血流量（GBF），但100mg/kg的大剂量则无效。CORM-2（5mg/kg和50mg/kg灌胃）显著增加胃黏膜CO含量和全血COHb水平。吲哚美辛、SC-560可逆转CORM-2诱导的保护作用，塞来昔布、ODQ和L-NNA则显著减弱该作用。血红素显著减轻乙醇损伤并增加GBF，而加剧乙醇诱导损伤的ZnPPIX则抑制CORM-2和血红素诱导的胃保护作用以及随之而来的GBF增加。CORM-2显著增加胃黏膜HO-1 mRNA表达，降低iNOS、IL-1β、COX-1和COX-2的mRNA表达，但未能影响乙醇降低的HO-1和Nrf2蛋白表达。我们得出结论，CORM-2释放的CO对乙醇诱导的胃损伤发挥胃保护作用，其机制包括通过sGC/环磷酸鸟苷（cGMP）、源自COX-1的前列腺素、NO-NO合酶系统介导的胃微循环增加及其抗炎特性。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/2265/4604159/c4cc5990fad6/pone.0140493.g001.jpg

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三羰基二氯钌（II）二聚体（CORM-2）释放的一氧化碳对实验性乙醇诱导的胃损伤的胃保护作用

Carbon Monoxide (CO) Released from Tricarbonyldichlororuthenium (II) Dimer (CORM-2) in Gastroprotection against Experimental Ethanol-Induced Gastric Damage.

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