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不同剂量的新生鼠氧气处理会改变小鼠的肺发育和对甲型流感病毒的宿主反应。

Lung development and the host response to influenza A virus are altered by different doses of neonatal oxygen in mice.

机构信息

Department of Environmental Medicine, School of Medicine and Dentistry, The University of Rochester, 601 Elmwood Ave., Rochester, NY 14642, USA.

出版信息

Am J Physiol Lung Cell Mol Physiol. 2012 May 15;302(10):L1078-87. doi: 10.1152/ajplung.00026.2012. Epub 2012 Mar 9.

Abstract

Oxygen exposure in preterm infants has been associated with altered lung development and increased risk for respiratory viral infections later in life. Although the dose of oxygen sufficient to exert these changes in humans remains unknown, adult mice exposed to 100% oxygen between postnatal days 1-4 exhibit alveolar simplification and increased sensitivity to influenza virus infection. Additionally, two nonlinear thresholds of neonatal oxygen exposures were previously identified that promote modest (between 40% and 60% oxygen) and severe (between 80% and 100% oxygen) changes in lung development. Here, we investigate whether these two thresholds correlate with the severity of lung disease following respiratory viral infection. Adult mice exposed to 100% oxygen at birth, and to a lesser extent 80% oxygen, demonstrated enhanced body weight loss, persistent inflammation, and fibrosis following infection compared with infected siblings exposed to room air at birth. In contrast, the host response to infection was indistinguishable between mice exposed to room air and 40% or 60% oxygen. Interestingly, levels of monocyte chemoattractant protein (MCP)-1 were equivalently elevated in infected mice that had been exposed to 80% or 100% oxygen as neonates. However, reducing levels of MCP-1 using heterozygous Mcp-1 mice did not affect oxygen-dependent changes in the response to infection. Thus lung development and the host response to respiratory viral infection are disrupted by different doses of oxygen. Our findings suggest that measuring lung function alone may not be sufficient to identify individuals born prematurely who have increased risk for respiratory viral infection.

摘要

早产儿暴露于氧气会导致肺部发育改变,并增加日后呼吸道病毒感染的风险。虽然目前尚不清楚足以引起人类发生这些变化的氧气剂量,但在出生后第 1-4 天暴露于 100%氧气的成年小鼠会出现肺泡简化和对流感病毒感染的敏感性增加。此外,先前已经确定了新生儿氧气暴露的两个非线性阈值,可促进适度(40%-60%氧气)和严重(80%-100%氧气)的肺部发育变化。在这里,我们研究了这两个阈值是否与呼吸道病毒感染后肺部疾病的严重程度相关。与出生时暴露于室内空气的感染同胞相比,出生时暴露于 100%氧气且在一定程度上暴露于 80%氧气的成年小鼠在感染后表现出体重减轻加重、持续炎症和纤维化。相比之下,出生时暴露于室内空气或 40%或 60%氧气的小鼠之间的宿主对感染的反应没有区别。有趣的是,作为新生儿暴露于 80%或 100%氧气的感染小鼠中单核细胞趋化蛋白 1(MCP-1)的水平同样升高。然而,使用杂合性 Mcp-1 小鼠降低 MCP-1 水平并没有影响感染时对氧气依赖的反应变化。因此,肺部发育和宿主对呼吸道病毒感染的反应受到不同剂量氧气的破坏。我们的研究结果表明,仅测量肺功能可能不足以识别有增加呼吸道病毒感染风险的早产儿。

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Low-dose hyperoxia primes airways for fibrosis in mice after influenza A infection.低剂量高氧预处理可增强甲型流感病毒感染后小鼠气道的纤维化。
Am J Physiol Lung Cell Mol Physiol. 2021 Oct 1;321(4):L750-L763. doi: 10.1152/ajplung.00289.2020. Epub 2021 Jul 29.

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Early CPAP versus surfactant in extremely preterm infants.极早产儿中早期 CPAP 与表面活性剂的比较。
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Target ranges of oxygen saturation in extremely preterm infants.极低出生体重儿氧饱和度目标范围。
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Distinct roles of FOXA2 and FOXA3 in allergic airway disease and asthma.FOXA2和FOXA3在变应性气道疾病和哮喘中的不同作用。
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