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卢西那肽可减轻 RDS 早产羊模型的肺部炎症反应,保护肺结构,并改善生理结局。

Lucinactant attenuates pulmonary inflammatory response, preserves lung structure, and improves physiologic outcomes in a preterm lamb model of RDS.

机构信息

Department of Physiology, Temple University School of Medicine, Philadelphia, Pennsylvania, USA.

出版信息

Pediatr Res. 2012 Oct;72(4):375-83. doi: 10.1038/pr.2012.96. Epub 2012 Jul 20.

Abstract

BACKGROUND

Acute inflammatory responses to supplemental oxygen and mechanical ventilation have been implicated in the pathophysiological sequelae of respiratory distress syndrome (RDS). Although surfactant replacement therapy (SRT) has contributed to lung stability, the effect on lung inflammation is inconclusive. Lucinactant contains sinapultide (KL4), a novel synthetic peptide that functionally mimics surfactant protein B, a protein with anti-inflammatory properties. We tested the hypothesis that lucinactant may modulate lung inflammatory response to mechanical ventilation in the management of RDS and may confer greater protection than animal-derived surfactants.

METHODS

Preterm lambs (126.8 ± 0.2 SD d gestation) were randomized to receive lucinactant, poractant alfa, beractant, or no surfactant and studied for 4 h. Gas exchange and pulmonary function were assessed serially. Lung inflammation biomarkers and lung histology were assessed at termination.

RESULTS

SRT improved lung compliance relative to no SRT without significant difference between SRT groups. Lucinactant attenuated lung and systemic inflammatory response, supported oxygenation at lower ventilatory requirements, and preserved lung structural integrity to a greater degree than either no SRT or SRT with poractant alfa or beractant.

CONCLUSION

These data suggest that early intervention with lucinactant may more effectively mitigate pulmonary pathophysiological sequelae of RDS than the animal-derived surfactants poractant alfa or beractant.

摘要

背景

补充氧气和机械通气引起的急性炎症反应与呼吸窘迫综合征(RDS)的病理生理后果有关。尽管表面活性剂替代疗法(SRT)有助于稳定肺部,但对肺部炎症的影响尚无定论。Lucinactant 含有 sinapultide(KL4),这是一种新型合成肽,可模拟具有抗炎特性的表面活性蛋白 B。我们假设 Lucinactant 可能会调节机械通气对 RDS 的肺部炎症反应,并比动物源性表面活性剂提供更大的保护作用。

方法

早产羔羊(126.8±0.2 SD d 孕龄)随机接受 Lucinactant、poractant alfa、beractant 或无表面活性剂治疗,并进行了 4 小时的研究。连续评估气体交换和肺功能。在研究结束时评估肺炎症生物标志物和肺组织学。

结果

SRT 改善了肺顺应性,与无 SRT 相比,但 SRT 组之间无显著差异。Lucinactant 减轻了肺和全身炎症反应,在较低的通气需求下支持氧合,并比无 SRT 或 SRT 加 poractant alfa 或 beractant 更能保护肺结构完整性。

结论

这些数据表明,早期干预用 Lucinactant 可能比动物源性表面活性剂 poractant alfa 或 beractant 更有效地减轻 RDS 的肺部病理生理后果。

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