Division of Perinatal Medicine, Yale University School of Medicine, Department of Pediatrics, Children's Hospital, 20 York Street, New Haven, CT 06520-8057, USA.
Am J Respir Cell Mol Biol. 2012 May;46(5):668-76. doi: 10.1165/rcmb.2011-0074OC. Epub 2012 Jan 6.
Supplemental oxygen is frequently prescribed. However, prolonged exposure to high concentrations of oxygen causes hyperoxic acute lung injury (HALI), which manifests as acute respiratory distress syndrome in adults and leads to bronchopulmonary dysplasia in newborns (NBs). Nitric oxide (NO), NO synthases (NOSs), and angiopoietin (Ang) 2 have been implicated in the pathogenesis of HALI. However, the mechanisms of the contributions of NOS/NO and the relationship(s) between NOS/NO and Ang2 have not been addressed. In addition, the relevance of these moieties in adults and NBs has not been evaluated. To address these issues, we compared the responses in hyperoxia of wild-type (NOS [+/+]) and NOS null (-/-) young adult and NB mice. When compared with NOS2(+/+) adult controls, NOS2(-/-) animals manifest exaggerated alveolar-capillary protein leak and premature death. These responses were associated with enhanced levels of structural cell death, enhanced expression of proapoptotic regulatory proteins, and Ang2. Importantly, silencing RNA knockdown of Ang2 decreased the levels of cell death and the expression of proapoptotic mediators. These effects were at least partially NOS2 specific, and were development dependent, because survival was similar in adult NOS3(+/+) and NOS3(-/-) mice and NB NOS2(+/+) and NOS2(-/-) mice, respectively. These studies demonstrate that NOS2 plays an important protective role in HALI in adult animals. They also demonstrate that this response is mediated, at least in part, by the ability of NOS2 to inhibit hyperoxia-induced Ang2 production and thereby decrease Ang2-induced tissue injury.
经常会开吸氧处方。然而,长时间暴露在高浓度氧气下会导致氧中毒性急性肺损伤(HALI),这会在成人中表现为急性呼吸窘迫综合征,并导致新生儿(NBs)出现支气管肺发育不良。一氧化氮(NO)、NO 合酶(NOSs)和血管生成素 2(Ang)已被认为与 HALI 的发病机制有关。然而,NOS/NO 的作用机制以及 NOS/NO 和 Ang2 之间的关系尚未得到解决。此外,这些物质在成人和 NBs 中的相关性尚未得到评估。为了解决这些问题,我们比较了野生型(NOS [+/+])和 NOS 缺失(-/-)年轻成年和 NB 小鼠在高氧环境中的反应。与 NOS2(+/+)成年对照相比,NOS2(-/-)动物表现出更明显的肺泡毛细血管蛋白渗漏和过早死亡。这些反应与结构细胞死亡水平升高、促凋亡调节蛋白表达增强和 Ang2 有关。重要的是,Ang2 的沉默 RNA 敲低降低了细胞死亡水平和促凋亡介质的表达。这些作用至少部分是 NOS2 特异性的,并且依赖于发育,因为成年 NOS3(+/+)和 NOS3(-/-)小鼠以及 NB NOS2(+/+)和 NOS2(-/-)小鼠的存活率相似。这些研究表明,NOS2 在成年动物的 HALI 中发挥重要的保护作用。它们还表明,这种反应至少部分是由 NOS2 抑制高氧诱导的 Ang2 产生的能力介导的,从而减少 Ang2 诱导的组织损伤。