Cancers (Feb 2022)

Identification of Early-Onset Metastasis in SF3B1 Mutated Uveal Melanoma

  • Wojtek Drabarek,
  • Job van Riet,
  • Josephine Q. N. Nguyen,
  • Kyra N. Smit,
  • Natasha M. van Poppelen,
  • Rick Jansen,
  • Eva Medico-Salsench,
  • Jolanda Vaarwater,
  • Frank J. Magielsen,
  • Tom Brands,
  • Bert Eussen,
  • Thierry. P. P. van den Bosch,
  • Robert M. Verdijk,
  • Nicole C. Naus,
  • Dion Paridaens,
  • Annelies de Klein,
  • Erwin Brosens,
  • Harmen J. G. van de Werken,
  • Emine Kilic,
  • on behalf of the Rotterdam Ocular Melanoma Study Group

DOI
https://doi.org/10.3390/cancers14030846
Journal volume & issue
Vol. 14, no. 3
p. 846

Abstract

Read online

Approximately 25% of all uveal melanoma (UM) contain driver mutations in the gene encoding the spliceosome factor SF3B1, and whilst patients with such SF3B1 mutations generally have an intermediate risk on developing metastatic disease, a third of these patients develop early metastasis within 5 years after diagnosis. We therefore investigated whether clinical and/or genetic variables could be indicative of short progression-free survival (PFS SF3B1-mutated (SF3B1mut) UM patients. We collected 146 SF3B1mut UM from our Rotterdam Ocular Melanoma Studygroup (ROMS) database and external published datasets. After stratification of all SF3B1mut UM using short PFS vs. long PFS, only largest tumor diameter (LTD) was significantly larger (mean: 17.7 mm (±2.8 SD) in the short PFS SF3B1mut group vs. the long PFS group (mean: 14.7 (±3.7 SD, p = 0.001). Combined ROMS and The Cancer Genome Atlas (TCGA) transcriptomic data were evaluated, and we identified SF3B1mut-specific canonical transcripts (e.g., a low expression of ABHD6 indicative for early-onset metastatic disease) or distinct expression of SF3B1mut UM aberrant transcripts, indicative of early- or late-onset or no metastatic SF3B1mut UM.

Keywords