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经气管内注射每日给药在早产兔肺部的局部递药:可行性和疗效。

Local pulmonary drug delivery in the preterm rabbit: feasibility and efficacy of daily intratracheal injections.

机构信息

Department of Development and Regeneration, Cluster Woman and Child, KU Leuven , Leuven , Belgium.

Facultad de Medicina, Universidad del Desarollo, Clínica Alemana, Santiago de Chile, Chile.

出版信息

Am J Physiol Lung Cell Mol Physiol. 2019 Apr 1;316(4):L589-L597. doi: 10.1152/ajplung.00255.2018. Epub 2019 Jan 24.

Abstract

Recent clinical trials in newborns have successfully used surfactant as a drug carrier for an active compound, to minimize systemic exposure. To investigate the translational potential of surfactant-compound mixtures and other local therapeutics, a relevant animal model is required in which intratracheal administration for maximal local deposition is technically possible and well tolerated. Preterm rabbit pups (born at 28 days of gestation) were exposed to either hyperoxia or normoxia and randomized to receive daily intratracheal surfactant, daily intratracheal saline, or no injections for 7 days. At day 7, the overall lung function and morphology were assessed. Efficacy in terms of distribution was assessed by micro-PET-CT on both day 0 and day 7. Lung function as well as parenchymal and vascular structure were altered by hyperoxia, thereby reproducing a phenotype reminiscent of bronchopulmonary dysplasia (BPD). Neither intratracheal surfactant nor saline affected the survival or the hyperoxia-induced BPD phenotype of the pups. Using PET-CT, we demonstrate that 82.5% of the injected radioactive tracer goes and remains in the lungs, with a decrease of only 4% after 150 min. Surfactant and saline can safely and effectively be administered in spontaneously breathing preterm rabbits. The described model and method enable researchers to evaluate intratracheal pharmacological interventions for the treatment of BPD.

摘要

最近在新生儿中的临床试验成功地将表面活性剂用作活性化合物的药物载体,以最大程度地减少全身暴露。为了研究表面活性剂-化合物混合物和其他局部治疗的转化潜力,需要一种相关的动物模型,该模型在技术上可以通过气管内给药来实现最大局部沉积,并且可以很好地耐受。将早产兔(胎龄 28 天出生)暴露于高氧或常氧中,并随机接受每日气管内表面活性剂、每日气管内生理盐水或 7 天不注射。在第 7 天,评估整体肺功能和形态。通过微 PET-CT 在第 0 天和第 7 天评估分布效果。肺功能以及实质和血管结构均被高氧改变,从而产生类似于支气管肺发育不良(BPD)的表型。气管内表面活性剂或生理盐水均未影响幼崽的存活或高氧诱导的 BPD 表型。使用 PET-CT,我们证明 82.5%的注射放射性示踪剂进入并留在肺部,150 分钟后仅减少 4%。表面活性剂和生理盐水可安全有效地用于自主呼吸的早产兔。所描述的模型和方法使研究人员能够评估用于治疗 BPD 的气管内药理干预。

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