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Effect of intermittent hypoxia or hyperoxia on lung development in preterm rat neonates during constant oxygen therapy

机译:间歇性缺氧或高氧对恒氧疗法早产大鼠新生儿肺发育的影响

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Abstract Impaired lung development is a major negative factor in the survival of preterm neonates. The present study was aimed to investigate the impact of constant oxygen, intermittent hyperoxia, and hypoxia on the lung development in preterm rat neonates. Neonatal rats were exposed to 40% O 2 with or without brief hyperoxia episodes (95% O 2 ) or brief hypoxia episodes (10% O 2 ) from day 0 to day 14, or to room air. The body weight, radical alveolar count (RAC), and total antioxidant capacity (TAOC) were significantly lower whereas the lung coefficient and malondialdehyde (MDA) were significantly higher in the hyperoxia and hypoxia groups than the air control and constant oxygen group at day 7, day 14, and day 21 after birth. The lung function indexes were reduced by intermittent hyperoxia and hypoxia. In contrast, the constant oxygen therapy increased the lung function. HIF‐1α and VEGF expression were significantly increased by hypoxia and decreased by hyperoxia. The constant oxygen therapy only decreased the HIF‐1α expression at day 14 and 21. In summary, the constant oxygen treatment promoted lung function without affecting the antioxidative capacity in preterm rat neonates. While intermittent hyperoxia and hypoxia inhibited lung development, decreased antioxidative capacity, and dysregulated HIF‐1α/VEGF signaling in preterm rat neonates.
机译:摘要肺部发展受损是早产新生儿的生存中的一个主要负面因素。目前的研究旨在调查恒定氧气,间歇性高氧和缺氧对早产大鼠新生儿肺部发育的影响。新生大鼠用或没有简短的高氧发作(95%O 2)或短暂的缺氧发作(10%O 2),或者在第0天或第14天或室内空气中暴露于40%的大鼠。体重,自由基肺泡计数(RAC)和总抗氧化能力(TAOC)显着降低,而肺系数和丙二醛(MDA)在7天的空气控制和常数氧气组中显着高于空气控制出生后第14天和第21天。间歇性高氧和缺氧减少了肺功能指标。相比之下,恒定的氧疗法增加了肺功能。 HIF-1α和VEGF表达被缺氧显着增加,并通过高氧降低。恒定的氧疗法仅降低了第14天和第21天的HIF-1α表达。总之,恒定的氧治疗促进了肺功能而不影响早产大鼠新生儿的抗氧化能力。虽然间歇性高氧和缺氧抑制肺部发育,降低抗氧化能力,并且在早产大鼠新生儿中减少了抗氧化能力和呼吸困难的HIF-1α/ VEGF信号传导。

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