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通过雾化途径对α1抗胰蛋白酶缺乏症进行雾化治疗的策略。

Strategies for aerosol therapy of alpha 1-antitrypsin deficiency by the aerosol route.

作者信息

Hubbard R C, Crystal R G

机构信息

Pulmonary Branch, National Heart, Lung, and Blood Institute, National Institutes of Health, Bethesda, Maryland 20892.

出版信息

Lung. 1990;168 Suppl:565-78. doi: 10.1007/BF02718179.

DOI:10.1007/BF02718179
PMID:2117165
Abstract

Alpha 1-antitrypsin (AAT) deficiency is a genetic disease in which low serum and lung levels of the antiprotease AAT cause a deficiency of the anti-elastase defensive screen of the lower respiratory tract such that neutrophil elastase is free to degrade the connective tissue of the lung, eventually resulting in emphysema. Intravenous AAT infusion therapy restores lung levels of AAT, but is inefficient, costly and a demanding form of therapy. As an alternative, we evaluated aerosol delivery of human plasma AAT (pAAT) and recombinant DNA-produced AAT (rAAT), as a means of providing anti-elastase protection to the lower respiratory tract. In vitro studies demonstrated that both pAAT and rAAT can be aerosolized into droplets suitable for alveolar deposition without loss of antiprotease activity. When administered by aerosol to individuals with AAT deficiency, pAAT and rAAT each significantly raised lung epithelial lining fluid levels of AAT and anti-neutrophil elastase capacity, with the likelihood that twice daily administration of 100 mg of either form would result in normalization of lung anti-elastase defenses at the alveolar surface. Studies in sheep further demonstrated that the aerosolized pAAT and rAAT were each able to pass through alveolar epithelium and gain access to the interstitial compartment of the lung, thus increasing anti-elastase defenses of the lung interstitium. Therapy was safe and well tolerated in all cases. Aerosol therapy with pAAT or rAAT is a safe, feasible, and likely a biochemically efficacious alternative to intravenous AAT augmentation therapy and merits further long-term studies for clinical therapy.

摘要

α1-抗胰蛋白酶(AAT)缺乏症是一种遗传性疾病,血清和肺中抗蛋白酶AAT水平较低会导致下呼吸道抗弹性蛋白酶防御屏障缺失,使得中性粒细胞弹性蛋白酶能够自由降解肺的结缔组织,最终导致肺气肿。静脉注射AAT输注疗法可恢复肺中AAT的水平,但效率低下、成本高昂且治疗要求苛刻。作为一种替代方法,我们评估了雾化递送人血浆AAT(pAAT)和重组DNA生产的AAT(rAAT),作为为下呼吸道提供抗弹性蛋白酶保护的一种手段。体外研究表明,pAAT和rAAT均可雾化成适合肺泡沉积的液滴,且不会丧失抗蛋白酶活性。当对AAT缺乏症患者进行雾化给药时,pAAT和rAAT均可显著提高肺上皮衬液中AAT的水平和抗中性粒细胞弹性蛋白酶能力,每天两次给予100 mg任何一种形式的AAT都有可能使肺泡表面的肺抗弹性蛋白酶防御恢复正常。在绵羊身上进行的研究进一步表明,雾化的pAAT和rAAT均能够穿过肺泡上皮并进入肺间质腔室,从而增强肺间质的抗弹性蛋白酶防御。在所有病例中,治疗都是安全的且耐受性良好。pAAT或rAAT雾化疗法是一种安全、可行且可能在生化方面有效的替代静脉注射AAT增强疗法的方法,值得进一步进行长期临床治疗研究。

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本文引用的文献

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Alpha 1 antitrypsin deficiency: the clinical and physiological features of pulmonary emphysema in subjects homozygous for Pi type Z. A survey by the British Thoracic Association.α1抗胰蛋白酶缺乏症:Pi型Z纯合子受试者肺气肿的临床和生理特征。英国胸科学会的一项调查。
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经表皮途径递送α1-抗胰蛋白酶疗法:值得探索。
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The design of a new truncated and engineered alpha1-antitrypsin based on theoretical studies: an antiprotease therapeutics for pulmonary diseases.基于理论研究设计新型截短型工程化α1-抗胰蛋白酶:一种用于肺部疾病的抗蛋白酶疗法。
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Lung deposition of inhaled alpha-1-proteinase inhibitor (alpha 1-PI) - problems and experience of alpha1-PI inhalation therapy in patients with hereditary alpha1-PI deficiency and cystic fibrosis.吸入的α-1-蛋白酶抑制剂(α1-PI)在肺部的沉积-遗传性α1-PI 缺乏症和囊性纤维化患者吸入α1-PI 治疗的问题和经验。
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Synthesis in E. coli of alpha 1-antitrypsin variants of therapeutic potential for emphysema and thrombosis.在大肠杆菌中合成对肺气肿和血栓形成具有治疗潜力的α1-抗胰蛋白酶变体。
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