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首页> 外文期刊>The European respiratory journal : >Lung deposition of inhaled alpha1-proteinase inhibitor in cystic fibrosis and alpha1-antitrypsin deficiency.
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Lung deposition of inhaled alpha1-proteinase inhibitor in cystic fibrosis and alpha1-antitrypsin deficiency.

机译:吸入性α1-蛋白酶抑制剂的肺沉积在囊性纤维化和α1-抗胰蛋白酶缺乏症中。

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摘要

Individuals with alpha(1)-antitrypsin (AAT) deficiency and cystic fibrosis (CF) have a protease-antiprotease imbalance in their lungs, which leads to early onset progressive lung disease. Inhalation of AAT may restore protective levels in the lungs. This study aimed to determine the efficiency of delivering AAT using a novel inhalation device in subjects with AAT deficiency and CF compared with healthy subjects. In total, 20 subjects (six healthy, seven with AAT deficiency and seven with CF) inhaled approximately 70 mg of radiolabelled active AAT, with controlled breathing patterns adjusted to lung function. Post-inhalation, total and regional lung deposition and extrathoracic deposition of radiolabelled AAT were measured. Total lung deposition of AAT was approximately 70% of the filling dose. The magnitude of deposition was similar in all treatment groups, with no adverse effect on lung function or any influence of disease severity on total lung deposition. Inhalation with controlled breathing patterns using the AKITA(2) device (lung function adapted) leads to high total lung deposition regardless of the degree of lung function impairment. Delivery of large amounts of AAT was achieved in a short period of time. This device may be an ideal option for aerosol therapy.
机译:患有α(1)-抗胰蛋白酶(AAT)缺乏症和囊性纤维化(CF)的个体的肺中存在蛋白酶-抗蛋白酶失衡,这会导致早期发作的进行性肺部疾病。吸入AAT可能会恢复肺部的保护水平。这项研究旨在确定与健康受试者相比,使用新型吸入装置在患有AAT缺乏和CF的受试者中提供AAT的效率。总共有20名受试者(六名健康,七名患有AAT缺乏症和七名患有CF)吸入约70 mg放射性标记的活性AAT,并根据肺功能调节了受控的呼吸方式。测量吸入后,放射性标记的AAT的全部和局部肺部沉积以及胸腔外沉积。 AAT在肺部的总沉积量约为充填剂量的70%。所有治疗组的沉积量均相似,对肺功能无不良影响或疾病严重程度对总肺沉积无任何影响。不论肺功能受损的程度如何,使用AKITA(2)设备(适应肺功能)以受控的呼吸方式进行吸入都会导致较高的总肺沉积。在短时间内实现了大量AAT的交付。该设备可能是气雾疗法的理想选择。

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