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Melatonin protects steatotic and nonsteatotic liver grafts against cold ischemia and reperfusion injury

机译:褪黑素可保护脂肪变性和非脂肪变性的肝移植物免受冷缺血和再灌注损伤

摘要

Chronic organ-donor shortage has required the acceptance of steatotic livers for transplantation purposes despite the higher risk of graft dysfunction or nonfunction associated with the cold ischemia-reperfusion injury. This study evaluated the use of melatonin as an additive to Institute Georges Lopez (IGL-1) solution for protecting nonsteatotic and steatotic liver grafts against cold ischemia-reperfusion injury. In the current investigation, we used an ex vivo isolated perfused rat liver model. Steatotic and nonsteatotic livers were preserved for 24 hr (4°C) in University of Wisconsin or IGL-1 solutions with or without melatonin, as well as in University of Wisconsin solution alone. Thereafter, livers were subjected to 2-hr reperfusion (37°C). We assessed hepatic injury (transaminases) and function [bile production and sulfobromophthalein (BSP) clearance, vascular resistance], as well as other factors potentially implicated in the high vulnerability of steatotic livers against ischemia-reperfusion injury (oxidative stress and related inflammatory mediators including nitric oxide and cytokines). We also evaluated well-known cytoprotective factors as hemeoxygenase 1 (HO-1). Fatty livers preserved in IGL-1 solution enriched with melatonin showed lower transaminase levels and higher bile production and BSP clearance when compared to those obtained for livers maintained in IGL-1 solution alone. A significant diminution of vascular resistance was also observed when melatonin was added to the IGL-1 solution. The melatonin benefits correlated with the generation of nitric oxide (through constitutive e-NOS activation) and the prevention of oxidative stress and inflammatory cytokine release including tumor necrosis factor and adiponectin, respectively. The addition of melatonin to IGL-1 solution improved nonsteatotic and steatotic liver graft preservation, limiting their risk against cold ischemia-reperfusion injury. © 2010 John Wiley & Sons A/S.
机译:尽管移植器官功能障碍或与冷缺血-再灌注损伤相关的功能障碍的风险较高,但慢性器官供体短缺已要求接受脂肪变性肝用于移植。这项研究评估了褪黑素作为乔治·洛佩兹研究所(IGL-1)溶液添加剂的用途,以保护非脂肪和脂肪变性的肝移植物免受冷缺血-再灌注损伤。在当前的研究中,我们使用了离体分离的灌流大鼠肝脏模型。威斯康星大学或含或不含褪黑激素的IGL-1溶液以及仅威斯康星大学溶液将脂肪变性和非脂肪变性肝脏保存24小时(4°C)。之后,对肝脏进行2小时再灌注(37°C)。我们评估了肝损伤(转氨酶)和功能[胆汁生成和磺基溴酞(BSP)清除率,血管阻力],以及可能与脂肪肝抵抗缺血-再灌注损伤的高脆弱性有关的其他因素(氧化应激和相关的炎症介质,包括一氧化氮和细胞因子)。我们还评估了众所周知的细胞保护因子,如血氧合酶1(HO-1)。与仅在IGL-1溶液中保存的肝脏相比,保存在富含褪黑激素的IGL-1溶液中保存的脂肪肝脏显示较低的转氨酶水平和较高的胆汁生成和BSP清除率。当将褪黑激素添加到IGL-1溶液中时,还观察到血管阻力的显着减少。褪黑激素的益处与一氧化氮的产生(通过本构性的e-NOS激活)以及防止氧化应激和炎症性细胞因子释放(包括肿瘤坏死因子和脂联素)有关。在IGL-1溶液中添加褪黑激素可改善非脂肪变性和脂肪变性肝移植物的保存,从而限制其抗冷缺血-再灌注损伤的风险。 ©2010 John Wiley&Sons A / S。

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