Marchand E, Verellen-Dumoulin C, Mairesse M, Delaunois L, Brancaleone P, Rahier J F, Vandenplas O
Service de Pneumologie, Cliniques Universitaires de Mont-Godinne, Université Catholique de Louvain, Yvoir, Belgium.
Chest. 2001 Mar;119(3):762-7. doi: 10.1378/chest.119.3.762.
To assess the frequency of cystic fibrosis transmembrane conductance regulator (CFTR) gene mutations in patients with allergic bronchopulmonary aspergillosis (ABPA).
Case-control study. All subjects in the study were screened for the presence of 13 mutations in the CFTR gene (R117H, 621 + 1G(-)>T, R334 W, Delta F508, Delta I507, 1717-1G(-)>A, G542X, R553X, G551D, R1162X, 3849 + 10kbC(-)>T, W1282X, and N1303K). Moreover, they were also screened for the presence of the 5T variant in intron 8.
University hospital and community-based hospital.
Twenty-one white patients with ABPA participated in the study. The presence of CFTR mutations was also investigated in 43 white subjects with allergic asthma who did not show sensitization to Aspergillus fumigatus and in 142 subjects seeking genetic counseling for diseases other than cystic fibrosis (CF).
Six patients with ABPA were found to be heterozygous for one CFTR mutation, including Delta F508 (n = 2), G542X (n = 1), R1162X (n = 1), 1717-1G(-)>A (n = 1), and R117H (n = 1). The 5T allele was not detected in ABPA patients. None of the ABPA patients showed sweat chloride concentrations > 60 mEq/L. The frequency of CFTR mutation carriers was significantly higher in ABPA patients (6 of 21 patients; 28.5%) than in control asthmatic subjects (2 of 43 subjects; 4.6%; p = 0.01) and in subjects seeking genetic counseling (6 of 142 subjects; p < 0.001).
These findings indicate that in patients without a clinical diagnosis of CF, CFTR gene mutations could be involved in the development of ABPA, in association with other genetic or environmental factors.
评估变应性支气管肺曲霉病(ABPA)患者中囊性纤维化跨膜传导调节因子(CFTR)基因突变的频率。
病例对照研究。对研究中的所有受试者进行CFTR基因13种突变(R117H、621 + 1G(-)>T、R334W、ΔF508、ΔI507、1717-1G(-)>A、G542X、R553X、G551D、R1162X、3849 + 10kbC(-)>T、W1282X和N1303K)的筛查。此外,还对他们进行第8内含子5T变异体的筛查。
大学医院和社区医院。
21例白人ABPA患者参与了研究。还对43例对烟曲霉无致敏反应的变应性哮喘白人受试者以及142例因除囊性纤维化(CF)以外的疾病寻求遗传咨询的受试者进行了CFTR基因突变情况的调查。
发现6例ABPA患者为一种CFTR基因突变的杂合子,包括ΔF508(n = 2)、G542X(n = 1)、R1162X(n = 1)、1717-1G(-)>A(n = 1)和R117H(n = 1)。在ABPA患者中未检测到5T等位基因。没有ABPA患者的汗液氯化物浓度>60 mEq/L。ABPA患者中CFTR突变携带者的频率(21例患者中的6例;28.5%)显著高于对照哮喘受试者(43例受试者中的2例;4.6%;p = 0.01)和寻求遗传咨询的受试者(142例受试者中的6例;p < 0.001)。
这些发现表明,在无CF临床诊断的患者中,CFTR基因突变可能与其他遗传或环境因素共同参与ABPA的发生发展。
