首页> 外文期刊>Journal of perinatology: Official journal of the California Perinatal Association >Patent ductus arteriosus hemodynamics in very premature infants treated with poractant alfa or beractant for respiratory distress syndrome.
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Patent ductus arteriosus hemodynamics in very premature infants treated with poractant alfa or beractant for respiratory distress syndrome.

机译:患有恶性呼吸窘迫综合征的婆婆或be婆治疗的早产儿动脉导管未闭的血流动力学。

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OBJECTIVE: Respiratory distress syndrome (RDS), requiring mechanical ventilation and exogenous surfactant treatment, and patent ductus arteriosus (PDA), are common co-morbidities in very premature infants. The effects of intra-tracheal surfactant administration on the cardiovascular and pulmonary systems in very premature infants with RDS and PDAs are not well characterized. We evaluated the effects of poractant alfa and beractant, surfactants with different rapidity of onset and duration of action, in very premature infants with RDS. To assess whether there were differences in PDA hemodynamics in very premature infants with RDS treated with poractant alfa and beractant during the first week of life and to assess whether poractant alfa or beractant had a direct effect on PDAs and PDA hemodynamics following the second dose of surfactant. STUDY DESIGN: We studied 50 in-born, very premature infants with RDS, 24 0 of 7 to 29 6 of 7 weeks gestation, treated with poractant alfa or beractant, in an open label, 1:1, randomized clinical trial. A subgroup of 16 patients with severe RDS, treated with a second dose of surfactant, had echocardiographical assessments before and 20 to 30 min after the second dose of surfactant. RESULT: There were 25 infants treated with poractant alfa (27.1+/-1.6 weeks, birth weight 930+/-231 g) and 25 treated with beractant (26.7+/-1.7 weeks, P=0.407 and birth weight 898+/-282 g, P=0.666). Clinically significant PDAs were diagnosed and treated in 8 of 25 (32%) of the poractant alfa and 19 of 25 (76%) of the beractant group (P=0.002). Indomethacin treatment was slightly earlier (3.4+/-2.5 days) in the poractant alfa than in the beractant group (5.1+/-4.9 days, P=0.038). Right ventricle pressure (RVP)/systolic arterial pressure (SAP) ratio in the first week was slightly lower in the poractant alfa (64+/-20%) than in the beractant (78+/-26%, P=0.048) group. Following a second dose of surfactant, neither poractant alfa nor beractant changed PDA flow. These hemodynamic observations were associated with less respiratory support in the poractant alfa group, allowing earlier extubation (13 of 25 at 48 h and 15 of 25 at 72 h), than in the beractant group (6 of 25 at 48 h, P=0.044, and 8 of 25 at 72 h, P=0.049). CONCLUSION: The more rapid improvement in pulmonary function in the poractant alfa-treated infants was associated with a lower RVP/SAP ratio and a corresponding earlier treatment with indomethacin. Neither surfactant had a significant direct effect on PDA hemodynamics. The lower frequency of clinically significant PDAs in the poractant alfa compared with the beractant group may represent an indirect effect of the differences in the pulmonary improvement induced by the two surfactants.
机译:目的:呼吸窘迫综合征(RDS)需要机械通气和外源性表面活性剂治疗,动脉导管未闭(PDA)是非常早产儿的常见合并症。还没有很好地表征气管内表面活性剂对非常早产RDS和PDA的婴儿对心血管和肺系统的影响。我们评估了早产儿RDS患儿α和fa药,具有不同起效速度和作用时间的表面活性剂的作用。评估在出生后的第一周内,接受早产儿阿尔法和beractant治疗的RDS早产儿的PDA血流动力学是否存在差异,并评估第二次使用表面活性剂后,阿尔法或beractant对其是否对PDA和PDA血流动力学有直接影响。研究设计:我们在开放标签的1:1随机临床试验中,对50例RDS,妊娠7周中的24 0至7到29 6中7胎的RDS早产婴儿进行了研究。用第二剂表面活性剂治疗的16名重度RDS患者的亚组在第二剂表面活性剂之前和之后20至30分钟进行了超声心动图评估。结果:25例接受阿尔法治疗的婴儿(27.1 +/- 1.6周,出生体重930 +/- 231 g)和25例接受了法术的婴儿(26.7 +/- 1.7周,P = 0.407,出生体重898 +/-) 282g,P = 0.666)。在有临床表现的PDA中,有25例(32%)的阿尔法和25例(25%)的19例被诊断和治疗(P = 0.002)。吲哚美辛的治疗时间(3.2 +/- 2.5天)在治疗性阿尔法患者中比在治疗者组(5.1 +/- 4.9天,P = 0.038)稍早。阿尔法(64 +/- 20%)患儿在第一周的右心室压力(RVP)/收缩期动脉压(SAP)的比率略低于观察者(78 +/- 26%,P = 0.048)组。在第二剂量的表面活性剂之后,辛辣的阿尔法和beractant都没有改变PDA流量。这些血液动力学观察结果与阿尔法练习组相比(练习48 h时25次中有6次,在48 h时25次中有6次,P = 0.044) ,以及在72 h时的25之8,P = 0.049)。结论:经阿尔法治疗的婴儿的肺功能改善更快,与较低的RVP / SAP比和相应的消炎痛治疗有关。两种表面活性剂都没有对PDA的血流动力学有明显的直接影响。与种植者相比,种植者阿尔法中具有临床意义的PDA频率更低,可能代表了两种表面活性剂引起的肺功能改善差异的间接影响。

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