Prevalence Estimates of Predicted Pathogenic COL4A3-COL4A5 Variants in a Population Sequencing Database and Their Implications for Alport Syndrome

Joel Gibson; Rachel Fieldhouse; Melanie M Y Chan; Omid Sadeghi-Alavijeh; Leslie Burnett; Valerio Izzi; Anton V Persikov; Daniel P Gale; Helen Storey; Judy Savige; Genomics England Research Consortium

doi:10.1681/ASN.2020071065

Prevalence Estimates of Predicted Pathogenic COL4A3-COL4A5 Variants in a Population Sequencing Database and Their Implications for Alport Syndrome

J Am Soc Nephrol. 2021 Sep;32(9):2273-2290. doi: 10.1681/ASN.2020071065. Epub 2021 Jun 18.

Authors

Affiliations

¹ The University of Melbourne Department of Medicine, Melbourne Health and Northern Health, Royal Melbourne Hospital, Parkville, Victoria, Australia.
² Kinghorn Centre for Clinical Genomics, Garvan Institute of Medical Research, Darlinghurst, New South Wales, Australia.
³ Department of Renal Medicine, University College London, London, United Kingdom.
⁴ Genomics England, Queen Mary University of London, London, United Kingdom.
⁵ Center for Cell-Matrix Research and Biocenter Oulu, University of Oulu, Oulu, Finland.
⁶ Lewis-Sigler Institute for Integrative Genomics, Princeton University, Princeton, New Jersey.
⁷ Molecular Genetics, Viapath Laboratories, Guy's Hospital, London, United Kingdom.

Abstract

Background: The reported prevalence of Alport syndrome varies from one in 5000 to one in 53,000 individuals. This study estimated the frequencies of predicted pathogenic COL4A3-COL4A5 variants in sequencing databases of populations without known kidney disease.

Methods: Predicted pathogenic variants were identified using filtering steps based on the ACMG/AMP criteria, which considered collagen IV α3-α5 position 1 Gly to be critical domains. The population frequencies of predicted pathogenic COL4A3-COL4A5 variants were then determined per mean number of sequenced alleles. Population frequencies for compound heterozygous and digenic combinations were calculated from the results for heterozygous variants.

Results: COL4A3-COL4A5 variants resulting in position 1 Gly substitutions were confirmed to be associated with hematuria (for each, P<0.001). Predicted pathogenic COL4A5 variants were found in at least one in 2320 individuals. p.(Gly624Asp) represented nearly half (16 of 33, 48%) of the variants in Europeans. Most COL4A5 variants (54 of 59, 92%) had a biochemical feature that potentially mitigated the clinical effect. The predicted pathogenic heterozygous COL4A3 and COL4A4 variants affected one in 106 of the population, consistent with the finding of thin basement membrane nephropathy in normal donor kidney biopsy specimens. Predicted pathogenic compound heterozygous variants occurred in one in 88,866 individuals, and digenic variants in at least one in 44,793.

Conclusions: The population frequencies for Alport syndrome are suggested by the frequencies of predicted pathogenic COL4A3-COL4A5 variants, but must be adjusted for the disease penetrance of individual variants and for the likelihood of already diagnosed disease and non-Gly substitutions. Disease penetrance may depend on other genetic and environmental factors.

Keywords: Alport syndrome; COL4A3; COL4A4; COL4A5; Gly substitutions; collagen IV; genetic renal disease; glomerular basement membrane; hematuria; thin basement membrane nephropathy.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Autoantigens / genetics*
Collagen Type IV / genetics*
Databases, Genetic
Female
Humans
Male
Mutation / genetics*
Nephritis, Hereditary / diagnosis
Nephritis, Hereditary / epidemiology*
Nephritis, Hereditary / genetics*
Penetrance
Prevalence

Substances

Autoantigens
COL4A5 protein, human
Collagen Type IV
type IV collagen alpha3 chain

Abstract

Publication types

MeSH terms

Substances

Grants and funding