Collagen type IV ‐related nephropathies in Portugal: pathogenic COL4A3 and COL4A4 mutations and clinical characterization of 25 families

Pathogenic mutations in genes COL4A3 / COL4A4 are responsible for autosomal Alport syndrome ( AS ) and thin basement membrane nephropathy ( TBMN ). We used Sanger sequencing to analyze all exons and splice site regions of COL4A3 / COL4A4 , in 40 unrelated Portuguese probands with clinical suspicion of AS / TBMN . To assess genotype–phenotype correlations, we compared clinically relevant phenotypes/outcomes between homozygous/compound heterozygous and apparently heterozygous patients. Seventeen novel and four reportedly pathogenic COL4A3 / COL4A4 mutations were identified in 62.5% (25/40) of the probands. Regardless of the mutated gene, all patients with ARAS manifested chronic renal failure ( CRF ) and hearing loss, whereas a minority of the apparently heterozygous patients had CRF or extrarenal symptoms. CRF was diagnosed at a significantly younger age in patients with ARAS . In our families, the occurrence of COL4A3 / COL4A4 mutations was higher, while the prevalence of XLAS was lower than expected. Overall, a pathogenic COL4A3 / COL4A4 / COL4A5 mutation was identified in >50% of patients with fewer than three of the standard diagnostic criteria of AS . With such a population background, simultaneous next‐generation sequencing of all three genes may be recommended as the most expedite approach to diagnose collagen IV ‐related glomerular basement membrane nephropathies.