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A variant in XPNPEP2 is associated with angioedema induced by angiotensin I-converting enzyme inhibitors
Authors:Duan Qing Ling  Nikpoor Borzoo  Dube Marie-Pierre  Molinaro Giuseppe  Meijer Inge A  Dion Patrick  Rochefort Daniel  Saint-Onge Judith  Flury Leah  Brown Nancy J  Gainer James V  Rouleau Jean L  Agostoni Angelo  Cugno Massimo  Simon Pierre  Clavel Pierre  Potier Jacky  Wehbe Bassem  Benarbia Seddik  Marc-Aurele Julien  Chanard Jacques  Foroud Tatiana  Adam Albert  Rouleau Guy A
Affiliation:Centre de recherche du CHUM, Hopital Notre-Dame, Montreal, Quebec, Canada.
Abstract:Angiotensin I-converting enzyme inhibitors (ACEi), which are used to treat common cardiovascular diseases, are associated with a potentially life-threatening adverse reaction known as angioedema (AE-ACEi). We have previously documented a significant association between AE-ACEi and low plasma aminopeptidase P (APP) activity. With eight large pedigrees, we hereby demonstrate that this quantitative trait is partially regulated by genetic factors. We tested APP activity using a variance-component QTL analysis of a 10-cM genomewide microsatellite scan enriched with seven markers over two candidate regions. We found significant linkage (LOD = 3.75) to a locus that includes the XPNPEP2 candidate gene encoding membrane-bound APP. Mutation screening of this QTL identified a large coding deletion segregating in one pedigree and an upstream single-nucleotide polymorphism (C-2399A SNP), which segregates in the remaining seven pedigrees. Measured genotype analysis strongly suggests that the linkage signal for APP activity at this locus is accounted for predominantly by the SNP association. In a separate case-control study (20 cases and 60 controls), we found significant association of this SNP to ACEi-induced AE (P=.0364). In conclusion, our findings provide supporting evidence that the C-2399A variant in XPNPEP2 is associated with reduced APP activity and a higher incidence of AE-ACEi.
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