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Alpha 1 antitrypsin distribution in an allergic asthmatic population sensitized to house dust mites
Authors:I. Suárez-Lorenzo  F. Rodríguez de Castro  D. Cruz-Niesvaara  E. Herrera-Ramos  C. Rodríguez-Gallego  T. Carrillo-Diaz
Affiliation:1.Postgraduate and Doctoral School,Universidad de Las Palmas de Gran Canaria,Las Palmas de Gran Canaria,Spain;2.Pneumology Unit,Hospital Universitario de Gran Canaria Doctor Negrín,Las Palmas de Gran Canaria,Spain;3.Allergy Unit,Hospital General de Fuerteventura,Puerto del Rosario,Spain;4.Immunology Unit,Hospital Universitario de Gran Canaria Doctor Negrín,Las Palmas de Gran Canaria,Spain;5.Allergy Unit,Hospital Universitario de Gran Canaria Doctor Negrín,Las Palmas de Gran Canaria,Spain
Abstract:

Background and objective

Severe alpha1 antitrypsin deficiency has been clearly associated with pulmonary emphysema, but its relationship with bronchial asthma remains controversial. Some deficient alpha 1 antitrypsin (AAT) genotypes seem to be associated with asthma development. The objective of this study was to analyze the distribution of AAT genotypes in asthmatic patients allergic to house dust mites (HDM), and to asses a possible association between these genotypes and severe asthma.

Methods

A cross-sectional cohort study of 648 patients with HDM allergic asthma was carried out. Demographic, clinical and analytical variables were collected. PI*S and PI*Z AAT deficient alleles of the SERPINA1 gene were assayed by real-time PCR.

Results

Asthma was intermittent in 253 patients and persistent in 395 patients (246 mild, 101 moderate and 48 severe). One hundred and forty-five asthmatic patients (22.4%) with at least one mutated allele (S or Z) were identified. No association between the different genotypes and asthma severity was found. No significant differences in all clinical and functional tests, as well as nasal eosinophils, IgA and IgE serum levels were observed. Peripheral eosinophils were significantly lower in patients with the PI*MS genotype (p?=?0.0228). Neither association between deficient AAT genotypes or serum ATT deficiency (AATD) and development of severe asthma, or correlation between ATT levels and FEV1 was observed.

Conclusion

In conclusion, the distribution of AAT genotypes in HDM allergic asthmatic patients did not differ from those found in Spanish population. Neither severe ATTD or deficient AAT genotypes appear to confer different clinical expression of asthma.
Keywords:
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