Klingbeil Lindsey R, Kim Paul, Piraino Giovanna, O'Connor Michael, Hake Paul W, Wolfe Vivian, Zingarelli Basilia
1 Department of Surgery, University of Cincinnati; and.
2 Division of Critical Care Medicine, Cincinnati Children's Hospital Medical Center, Cincinnati, Ohio.
Am J Respir Cell Mol Biol. 2017 May;56(5):585-596. doi: 10.1165/rcmb.2016-0118OC.
The development of multiple organ failure in patients with hemorrhagic shock is significantly influenced by patient age. Adenosine monophosphate-activated protein kinase (AMPK) is a crucial regulator of energy homeostasis, which coordinates metabolic repair during cellular stress. We investigated whether AMPK-regulated signaling pathways are age-dependent in hemorrhage-induced lung injury and whether AMPK activation by 5-amino-4-imidazole carboxamide riboside (AICAR) affords lung protective effects. Male C57/BL6 young mice (3-5 mo), mature adult mice (9-12 mo), and young AMPKα1 knockout mice (3-5 mo) were subjected to hemorrhagic shock by blood withdrawing, followed by resuscitation with shed blood and lactated Ringer's solution. Plasma proinflammatory cytokines were similarly elevated in C57/BL6 young and mature adult mice after hemorrhagic shock. However, mature adult mice exhibited more severe lung edema and neutrophil infiltration, and higher mitochondrial damage in alveolar epithelial type II cells, than did young mice. No change in autophagy was observed. At molecular analysis, the phosphorylation of the catalytic subunit AMPKα1 was associated with nuclear translocation of peroxisome proliferator-activated receptor γ co-activator-α in young, but not mature, adult mice. Treatment with AICAR ameliorated the disruption of lung architecture in mice of both ages; however, effects in mature adult mice were different than young mice and also involved inhibition of nuclear factor-κB. In young AMPKα1 knockout mice, AICAR failed to improve hypotension and lung neutrophil infiltration. Our data demonstrate that during hemorrhagic shock, AMPK-dependent metabolic repair mechanisms are important for mitigating lung injury. However, these mechanisms are less competent with age.
失血性休克患者多器官功能衰竭的发生发展受患者年龄的显著影响。单磷酸腺苷激活蛋白激酶(AMPK)是能量稳态的关键调节因子,在细胞应激期间协调代谢修复。我们研究了AMPK调节的信号通路在出血性肺损伤中是否存在年龄依赖性,以及5-氨基-4-咪唑甲酰胺核苷(AICAR)激活AMPK是否具有肺保护作用。雄性C57/BL6幼鼠(3 - 5月龄)、成年小鼠(9 - 12月龄)和幼龄AMPKα1基因敲除小鼠(3 - 5月龄)通过放血诱导失血性休克,随后用自体血和乳酸林格氏液进行复苏。失血性休克后,C57/BL6幼鼠和成年小鼠血浆促炎细胞因子水平同样升高。然而,成年小鼠比幼鼠表现出更严重的肺水肿和中性粒细胞浸润,以及肺泡II型上皮细胞中更高的线粒体损伤。未观察到自噬的变化。分子分析显示,催化亚基AMPKα1的磷酸化与幼龄成年小鼠而非成年成年小鼠中过氧化物酶体增殖物激活受体γ共激活因子-α的核转位有关。用AICAR治疗可改善两个年龄段小鼠的肺结构破坏;然而,对成年成年小鼠的作用与幼鼠不同,还涉及对核因子-κB的抑制。在幼龄AMPKα1基因敲除小鼠中,AICAR未能改善低血压和肺中性粒细胞浸润。我们的数据表明,在失血性休克期间,AMPK依赖的代谢修复机制对减轻肺损伤很重要。然而,这些机制随年龄增长而功能减弱。