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PMID 9272157
Gene Name CFTR
Condition Congenital absence of the vas deferens (CAVD)
Association  Clinical examination of patients with CFTR mutations on both chromosomes revealed elevated sweat chloride concentrations and discrete symptoms of respiratory disease in a subset of patients. Thus, our collaborative study shows that CAVD without renal mal
Mutation  delta F508, R117H
Population size 106
Population details 106 CAVD
Sex Male
Infertility type Male infertility
Other associated phenotypes Congenital bilateral absence of the vas deferens, cystic fibrosis


Distinct spectrum of CFTR gene mutations in congenital absence of vas deferens

Dörk T, Dworniczak B, Aulehla-Scholz C, Wieczorek D, Böhm I, Mayerova A, Seydewitz HH, Nieschlag E, Meschede D, Horst J, Pander HJ, Sperling H, Ratjen F, Passarge E, Schmidtke J, Stuhrmann M.

Congenital absence of the vas deferens (CAVD) is a frequent cause for obstructive azoospermia and accounts for 1%-2% of male infertility. A high incidence of mutations of the cystic fibrosis transmembrane conductance regulator (CFTR) gene has recently been reported in males with CAVD. We have investigated a cohort of 106 German patients with congenital bilateral or unilateral absence of the vas deferens for mutations in the coding region, flanking intron regions and promotor sequences of the CFTR gene. Of the CAVD patients, 75% carried CFTR mutations or disease-associated CFTR variants, such as the "5T" allele, on both chromosomes. The distribution of mutation genotypes clearly differed from that observed in cystic fibrosis. None of the CAVD patients was homozygous for delta F508 and none was compound heterozygous for delta F508 and a nonsense or frameshift mutation. Instead, homozygosity was found for a few mild missense or splicing mutations, and the majority of CAVD mutations were missense substitutions. Twenty-one German CAVD patients were compound heterozygous for delta F508 and R117H, which was the most frequent CAVD genotype in our study group. Haplotype analysis indicated a common origin for R117H in our population, whereas another frequent CAVD mutation, viz. the "5T allele" was a recurrent mutation on different intragenic haplotypes and multiple ethnic backgrounds. We identified a total of 46 different mutations and variants, of which 15 mutations have not previously been reported. Thirteen novel missense mutations and one unique amino-acid insertion may be confined to the CAVD phenotype. A few splice or missense variants, such as F508C or 1716 G-->A, are proposed here as possible candidate CAVD mutations with an apparently reduced penetrance. Clinical examination of patients with CFTR mutations on both chromosomes revealed elevated sweat chloride concentrations and discrete symptoms of respiratory disease in a subset of patients. Thus, our collaborative study shows that CAVD without renal malformation is a primary genital form of cystic fibrosis in the vast majority of German patients and links the particular expression of clinical symptoms in CAVD with a distinct subset of CFTR mutation genotypes. FAU - Dörk, T AU - Dörk T AD - Institut für Humangenetik, Medizinische Hochschule Hannover, Germany. FAU - Dworniczak, B AU - Dworniczak B FAU - Aulehla-Scholz, C AU - Aulehla-Scholz C FAU - Wieczorek, D AU - Wieczorek D FAU - Böhm, I AU - Böhm I FAU - Mayerova, A AU - Mayerova A FAU - Seydewitz, H H AU - Seydewitz HH FAU - Nieschlag, E AU - Nieschlag E FAU - Meschede, D AU - Meschede D FAU - Horst, J AU - Horst J FAU - Pander, H J AU - Pander HJ FAU - Sperling, H AU - Sperling H FAU - Ratjen, F AU - Ratjen F FAU - Passarge, E AU - Passarge E FAU - Schmidtke, J AU - Schmidtke J