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α 1 -Antitrypsin deficiency and chronic respiratory disorders

机译:α1-丙烯酸辛缺乏症和慢性呼吸系统障碍

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α 1 -antitrypsin deficiency (AATD) is a hereditary disorder associated with a risk of developing liver disease and pulmonary emphysema, and other chronic respiratory disorders (mainly asthma and bronchiectasis); Z variant is the commonest deficient variant of AAT. Determining AAT concentration in serum or plasma and identifying allelic variants by phenotyping or genotyping are fundamental in the diagnosis of AATD. Initial evaluation and annual follow-up measurement of lung function, including post-bronchodilator forced expiratory volume in 1?s and gas transfer inform on disease progression. Lung densitometry is the most sensitive measure of emphysema progression, but must not be use in the follow-up of patients in routine clinical practice. The exogenous administration of purified human serum-derived AAT is the only approved specific treatment for AATD in PiZZ. AAT augmentation therapy is not recommended in PiSZ, PiMZ or current smokers of any protein phenotype, or in patients with hepatic disease. Lung volume reduction and endoscopic bronchial valve placement are useful in selected patients, whereas the survival benefit of lung transplant is unclear. There are several new lines of research in AATD to improve the diagnosis and evaluation of the response to therapy and to develop genetic and regenerative therapies and other treatments.
机译:α1-乙醛缺乏(AATD)是一种遗传性疾病,其与发育肝病和肺气肿的风险以及其他慢性呼吸道疾病(主要是哮喘和支气管扩张); Z变体是AAT的最常见的缺陷变体。确定血清或血浆中的AAT浓度,并通过表型或基因分型鉴定等位基因变体是AATD诊断的基础。肺功能的初步评估和年后续测量,包括核心偶联剂强制呼气量,在1?S和天然气转移通知疾病进展。肺密度测定是肺气肿进展最敏感的措施,但不能在常规临床实践中的患者随访中使用。外源性纯化的人血清衍生的AAT给药是PIZZ中唯一批准的AATD特异性处理。不推荐在PISZ,PIMZ或目前任何蛋白质表型的吸烟者或肝脏疾病患者中推荐AAT增强治疗。肺体积减小和内窥镜支气管瓣膜放置在选定的患者中是有用的,而肺移植的存活效果尚不清楚。 AATD中有几种新的研究态度,改善对治疗的响应的诊断和评估,以及发展遗传和再生治疗和其他治疗。

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