共查询到11条相似文献,搜索用时 0 毫秒
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Alexis S. Davis Susan R. Hintz Krisa P. Van Meurs Lei Li Abhik Das Barbara J. Stoll Michele C. Walsh Athina Pappas Edward F. Bell Abbot R. Laptook Rosemary D. Higgins Eunice Kennedy Shriver National Institute of Child Health Human Development Neonatal Research Network 《The Journal of pediatrics》2010,157(5):720-725
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Hintz SR Van Meurs KP Perritt R Poole WK Das A Stevenson DK Ehrenkranz RA Lemons JA Vohr BR Heyne R Childers DO Peralta-Carcelen M Dusick A Johnson YR Morris B Dillard R Vaucher Y Steichen J Adams-Chapman I Konduri G Myers GJ de Ungria M Tyson JE Higgins RD;NICHD Neonatal Research Network 《The Journal of pediatrics》2007,151(1):16-22
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Hascoet JM Fresson J Claris O Hamon I Lombet J Liska A Cantagrel S Al Hosri J Thiriez G Valdes V Vittu G Egreteau L Henrot A Buchweiller MC Onody P 《The Journal of pediatrics》2005,146(3):318-323
OBJECTIVES: To assess the safety-efficacy balance of low-dose inhaled nitric oxide (iNO) in hypoxemic premature infants because no sustained beneficial effect has been demonstrated clearly and there are concerns about side effects. STUDY DESIGN: Eight hundred and sixty infants <32 weeks were randomized at birth to receive 5 ppm iNO or placebo when they presented with hypoxemic respiratory failure (HRF) defined by a requirement for mechanical ventilation, fraction of inspired oxygen (FIO 2 ) >40%, and arterio-alveolar ratio in oxygen (aAO 2 ) <0.22. The primary end point was intact survival at 28 days of age. RESULTS: Sixty-one of 415 infants presented with HRF and were compared with 84 of 445 controls who presented with HRF. There was no difference in the primary end point (61.4% in infants [23% with HRF who were treated with iNO] vs 61.1% in controls [21.4% in controls with HRF]; P = .943). For the infants with HRF who were treated with iNO, there was no significant difference from controls for intraventricular hemorrhage (IVH) (6% vs 7%), necrotizing enterocolitis (8% vs 6 %), or patent ductus arteriosus (PDA) (34% vs 37%). Compared with nonhypoxemic infants, the risk of bronchopulmonary displasia (BPD) increased significantly in HRF controls (OR = 3.264 [CI 1.461-7.292]) but not in infants with HRF who were treated with iNO (OR = 1.626 [CI 0.633-4.178]). CONCLUSIONS: iNO appears to be safe in premature infants but did not lead to a significant improvement in intact survival on day 28. 相似文献