A novel COL4A5 mutation identified in a Chinese Han family using exome sequencing.

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Alport syndrome (AS ) is a monogenic disease of the basement membrane (BM ), resulting in progressive renal failure due to glomerulonephropathy , variable sensorineural hearing loss , and ocular anomalies . It is caused by mutations in the collagen type IV alpha-3 gene (COL 4 A 3 ), the collagen type IV alpha-4 gene (COL 4 A 4 ), and the collagen type IV alpha-5 gene (COL 4 A 5 ), which encodes type IV collagen α 3 , α 4 , and α 5 chains , respectively . To explore the disease-related gene in a four -generation Chinese Han pedigree of AS , exome sequencing was conducted on the proband , and a novel deletion mutation c .499 delC (p .Pro 167 Glnfs *36 ) in the COL 4 A 5 gene was identified . This mutation , absent in 1 ,000 genomes project , HapMap , dbSNP 132 , YH 1 databases , and 100 normal controls , cosegregated with patients in the family . Neither sensorineural hearing loss nor typical COL 4 A 5 -related ocular abnormalities (dot-and-fleck retinopathy , anterior lenticonus , and the rare posterior polymorphous corneal dystrophy ) were present in patients of this family . The phenotypes of patients in this AS family were characterized by early onset-age and rapidly developing into end-stage renal disease (ESRD ). Our discovery broadens the mutation spectrum in the COL 4 A 5 gene associated with AS , which may also shed new light on genetic counseling for AS .