npj Genomic Medicine (Jan 2022)

Evidence that the Ser192Tyr/Arg402Gln in cis Tyrosinase gene haplotype is a disease-causing allele in oculocutaneous albinism type 1B (OCA1B)

  • Siying Lin,
  • Aida Sanchez-Bretaño,
  • Joseph S. Leslie,
  • Katie B. Williams,
  • Helena Lee,
  • N. Simon Thomas,
  • Jonathan Callaway,
  • James Deline,
  • J. Arjuna Ratnayaka,
  • Diana Baralle,
  • Melanie A. Schmitt,
  • Chelsea S. Norman,
  • Sheri Hammond,
  • Gaurav V. Harlalka,
  • Sarah Ennis,
  • Harold E. Cross,
  • Olivia Wenger,
  • Andrew H. Crosby,
  • Emma L. Baple,
  • Jay E. Self

DOI
https://doi.org/10.1038/s41525-021-00275-9
Journal volume & issue
Vol. 7, no. 1
pp. 1 – 11

Abstract

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Abstract Oculocutaneous albinism type 1 (OCA1) is caused by pathogenic variants in the TYR (tyrosinase) gene which encodes the critical and rate-limiting enzyme in melanin synthesis. It is the most common OCA subtype found in Caucasians, accounting for ~50% of cases worldwide. The apparent ‘missing heritability’ in OCA is well described, with ~25–30% of clinically diagnosed individuals lacking two clearly pathogenic variants. Here we undertook empowered genetic studies in an extensive multigenerational Amish family, alongside a review of previously published literature, a retrospective analysis of in-house datasets, and tyrosinase activity studies. Together this provides irrefutable evidence of the pathogenicity of two common TYR variants, p.(Ser192Tyr) and p.(Arg402Gln) when inherited in cis alongside a pathogenic TYR variant in trans. We also show that homozygosity for the p.(Ser192Tyr)/p.(Arg402Gln) TYR haplotype results in a very mild, but fully penetrant, albinism phenotype. Together these data underscore the importance of including the TYR p.(Ser192Tyr)/p.(Arg402Gln) in cis haplotype as a pathogenic allele causative of OCA, which would likely increase molecular diagnoses in this missing heritability albinism cohort by 25–50%.