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在胎粪吸入综合征兔模型中,用布地奈德强化外源性表面活性剂治疗后的肺部炎症和氧化改变。

Lung inflammatory and oxidative alterations after exogenous surfactant therapy fortified with budesonide in rabbit model of meconium aspiration syndrome.

作者信息

Mikolka P, Kopincová J, Košútová P, Čierny D, Čalkovská A, Mokrá D

机构信息

Biomedical Center Martin and Department of Physiology, Jessenius Faculty of Medicine in Martin, Comenius University in Bratislava, Martin, Slovak Republic.

出版信息

Physiol Res. 2016 Dec 22;65(Suppl 5):S653-S662. doi: 10.33549/physiolres.933529.

DOI:10.33549/physiolres.933529
PMID:28006947
Abstract

Meconium aspiration syndrome (MAS) triggers inflammatory and oxidative pathways which can inactivate both pulmonary surfactant and therapeutically given exogenous surfactant. Glucocorticoid budesonide added to exogenous surfactant can inhibit inflammation and thereby enhance treatment efficacy. Neonatal meconium (25 mg/ml, 4 ml/kg) was administered intratracheally (i.t.) to rabbits. When the MAS model was prepared, animals were treated with budesonide i.t. (Pulmicort, 0.25 mg/kg, M+B); with surfactant lung lavage (Curosurf®, 10 ml/kg, 5 mg phospholipids/ml, M+S) followed by undiluted Curosurf® i.t. (100 mg phospholipids/kg); with combination of budesonide and surfactant (M+S+B); or were untreated (M); or served as controls with saline i.t. instead of meconium (C). Animals were oxygen-ventilated for additional 5 h. Cell counts in the blood and bronchoalveolar lavage fluid (BAL), lung edema formation (wet/dry weight ratio), oxidative damage of lipids/ proteins and inflammatory expression profiles (IL-2, IL-6, IL-13, TNF-alpha) in the lung homogenate and plasma were determined. Combined surfactant+budesonide therapy was the most effective in reduction of neutrophil counts in BAL, oxidative damage, levels and mRNA expression of cytokines in the lung, and lung edema formation compared to untreated animals. Curosurf fortified with budesonide mitigated lung inflammation and oxidative modifications what indicate the perspectives of this treatment combination for MAS therapy.

摘要

胎粪吸入综合征(MAS)会引发炎症和氧化途径,这可能会使肺表面活性物质以及治疗时给予的外源性表面活性物质失活。将糖皮质激素布地奈德添加到外源性表面活性物质中可以抑制炎症,从而提高治疗效果。将新生兔的胎粪(25毫克/毫升,4毫升/千克)经气管内(i.t.)给药。制备MAS模型时,对动物进行气管内布地奈德治疗(普米克,0.25毫克/千克,M+B);进行表面活性物质肺灌洗(珂立苏®,10毫升/千克,5毫克磷脂/毫升,M+S),随后经气管内给予未稀释的珂立苏®(100毫克磷脂/千克);进行布地奈德和表面活性物质联合治疗(M+S+B);或不进行治疗(M);或用生理盐水经气管内给药代替胎粪作为对照(C)。动物再进行5小时的氧气通气。测定血液和支气管肺泡灌洗液(BAL)中的细胞计数、肺水肿形成(湿/干重比)、肺匀浆和血浆中脂质/蛋白质的氧化损伤以及炎症表达谱(IL-2、IL-6、IL-13、TNF-α)。与未治疗的动物相比,表面活性物质+布地奈德联合治疗在降低BAL中的中性粒细胞计数、氧化损伤、肺中细胞因子水平和mRNA表达以及肺水肿形成方面最为有效。用布地奈德强化的珂立苏减轻了肺部炎症和氧化修饰,这表明这种治疗组合在MAS治疗方面具有前景。

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