Emphysema due to α-antitrypsin deficiency: Familial study of the YBARCELONA variant

A 39-year-old female patient, an ex-smoker with an 8-pack-year smoking history and severe pulmonary emphysema of early onset, received a diagnosis of alpha(1)-antitrypsin (AAT) deficiency and proved to be a carrier of a new deficient variant, YBARCELONA, derived from the normal M1 variant with two s...

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Published inChest Vol. 124; no. 1; pp. 404 - 406
Main Authors MIRAVITLLES, Marc, VILA, Sara, JARDI, Rosendo, DE LA ROZA, Cristian, RODRIGUEZ-FRIAS, Francisco, VIDAL, Rafael
Format Journal Article
LanguageEnglish
Published Northbrook, IL American College of Chest Physicians 01.07.2003
Subjects
Adult
alpha 1-Antitrypsin Deficiency - complications
alpha 1-Antitrypsin Deficiency - diagnosis
alpha 1-Antitrypsin Deficiency - genetics
Biological and medical sciences
Female
Follow-Up Studies
Genetic Variation
Heterozygote
Humans
Male
Medical sciences
Pneumology
Pulmonary Emphysema - diagnosis
Pulmonary Emphysema - genetics
Respiratory Function Tests
Respiratory system : syndromes and miscellaneous diseases
Smoking - adverse effects
Time Factors
Human
Lung disease
Respiratory disease
Family study
Pathogenesis
Deficiency
Genetic variant
pulmonary emphysema
Glycoprotein
Metabolic diseases
Genotype
Enzymopathy
Genetic determinism
YBARCFILONA
α1-antitnpsin deficiency
α1-Antitrypsin
Genetic disease
Case study
Phenotype
Lung function
Bronchus disease
Obstructive pulmonary disease
Emphysema
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ISSN0012-3692
DOI10.1378/chest.124.1.404

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Summary:A 39-year-old female patient, an ex-smoker with an 8-pack-year smoking history and severe pulmonary emphysema of early onset, received a diagnosis of alpha(1)-antitrypsin (AAT) deficiency and proved to be a carrier of a new deficient variant, YBARCELONA, derived from the normal M1 variant with two substitutions: one in exon III and the other in exon V. AAT genotype of eight members of the same family and study of lung function of the index case and family members at baseline and after 6 years of follow-up were performed. Five subjects were PiYM, with intermediate serum AAT concentrations and normal pulmonary function. No changes were observed over 6 years in pulmonary function of the PiYM patients who were nonsmokers; however, the PiYY index case presented worsening of pulmonary function with FEV(1) of 33%. The heterozygotes PiYM have AAT concentrations similar to the PiMZ and, at 6 years, the nonsmokers presented no worsening in pulmonary function. The risk associated with this variant in its heterozygous form may be similar to that described for PiMZ.
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ISSN:0012-3692
DOI:10.1378/chest.124.1.404