Dopachrome tautomerase variants in patients with oculocutaneous albinism

Author:

Pennamen Perrine,Tingaud-Sequeira Angèle,Gazova Iveta,Keighren Margaret,McKie Lisa,Marlin Sandrine,Halem Souad Gherbi,Kaplan Josseline,Delevoye Cédric,Lacombe Didier,Plaisant Claudio,Michaud Vincent,Lasseaux Eulalie,Javerzat Sophie,Jackson IanORCID,Arveiler Benoit

Abstract

ABSTRACTPurposeAlbinism is a clinically and genetically heterogeneous condition. Despite analysis of the nineteen known genes, ∼30% patients remain unsolved. We aimed to identify new genes involved in albinism.MethodsWe sequenced a panel of genes with known or predicted involvement in melanogenesis in 230 unsolved albinism patients.ResultsWe identified variants in the Dopachrome tautomerase (DCT) gene in two patients. One was compound heterozygous for a 14 bp deletion in exon 9 and c.118T>A p.(Cys40Ser). The second was homozygous for c.183C>G p.(Cys61Trp). Both patients had mild hair and skin hypopigmentation, and classical ocular features. CRISPR/Cas9 was used in C57BL/6J mice to create mutations identical to the missense mutations carried by the patients, along with one loss-of-function indel mutation. When bred to homozygosity the three mutations revealed hypopigmentation of the coat, milder for Cys40Ser compared to Cys61Trp or the frameshift mutation. Histological analysis identified significant hypopigmentation of the retinal pigmented epithelium (RPE) indicating that defective RPE melanogenesis could be associated with eye and vision defects. DCT loss of function in zebrafish embryos elicited hypopigmentation both in melanocytes and RPE cells.ConclusionsDCT is the gene for a new type of oculocutaneous albinism that we propose to name OCA8.

Publisher

Cold Spring Harbor Laboratory

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