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Germline Variants in Patients Affected by Both Uveal and Cutaneous Melanoma

  • Peter A. Johansson
  • , Jane M. Palmer
  • , Lindsay McGrath
  • , Sunil Warrier
  • , Hayley R. Hamilton
  • , Timothy Beckman
  • , Matthew G. D'Mellow
  • , Kelly M. Brooks
  • , William Glasson
  • , Nicholas K. Hayward
  • , Antonia L. Pritchard

Résultats de recherche: ArticleRevue par des pairs

5 Citations (Scopus)

Résumé

Uveal melanoma (UM) and nonacral cutaneous melanoma (CM) are distinct entities with varied genetic landscapes despite both arising from melanocytes. There are, however, similarities in that they most frequently affect people of European ancestry, and high penetrance germline variants in BAP1, POT1 and CDKN2A have been shown to predispose to both UM and CM. This study aims to further explore germline variants in patients affected by both UM and CM, shedding light on the underlying genetic mechanism causing these diseases. Using exome sequencing we analysed germline DNA samples from a cohort of 83 Australian patients diagnosed with both UM and CM. Eight (10%) patients were identified that carried pathogenic mutations in known melanoma predisposition genes POT1, MITF, OCA2, SLC45A2 and TYR. Three (4%) patients carried pathogenic variants in genes previously linked with other cancer syndromes (ATR, BRIP1 and MSH6) and another three cases carried monoallelic pathogenic variants in recessive cancer genes (xeroderma pigmentosum and Fanconi anaemia), indicating that reduced penetrance of phenotype in these individuals may contribute to the development of both UM and CM. These findings highlight the need for further studies characterising the role of these genes in melanoma susceptibility.

langue originaleEnglish
Numéro d'articlee13199
journalPigment Cell and Melanoma Research
Volume38
Numéro de publication1
Les DOIs
étatPublished - 24 sept. 2024

SDG des Nations Unies

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