Table 2.
Uveal melanoma driver genes and their prognostic significance
| Gene | Gene function | Mutation frequency (%) | Association with metastases | Association with survival |
|---|---|---|---|---|
| GNAQ | Mediating signalling between G‐protein‐coupled receptors and downstream effectors and upregulated MAPK pathway | 43–57 | Similar frequencies reported between metastatic and non‐metastatic lesions | Mutations have not been linked to patient outcome 113 |
| GNA11 | Mediating signalling between G‐protein‐coupled receptors and downstream effectors and upregulated MAPK pathway | 41–49 | Present in 18/30 (60%) of UM metastases | Disease‐specific survival in GNA11‐mutant patients was 60 months, overall survival 50.6 months (from date of primary tumour), significantly poorer than those tumours lacking GNA11 mutations 117 |
| BAP1 | Involved in tumour suppression, DNA damage response and proliferation | 70–83 | Inactivating somatic mutations in 26/31 (84%) of metastasising tumours. Also associated with Class 2 GEP, M3 and 8q gain. | Overall survival in BAP1 positive nuclear staining by IHC was 9.97 months (95% confidence interval 8.05–11.9) versus BAP1 negative by IHC 4.74 (3.49–6.0) 49, 118, 119 |
| EIF1AX | Eukaryotic translation initiation factor | 8–21 | Mutant cases are associated with very low risk of metastases (only 2/28 cases) | EIF1AX mutant cases had a longer disease‐free survival than EIF1AX non‐mutant cases (190.1 vs. 100.2 months; p < 0.001) 113, 120, 121 |
| SF3B1 | Required for pre‐mRNA splicing | 10–24 | Intermediate risk of metastases – late‐onset (>5 years) metastases can occur | Although an association of mutated SF3B1 with favourable prognosis was observed in the first few years 122, with longer follow up time, SF3B1 mutant patients developed more metastases and tumours with D3 and SF3B1 mutation showed a significant worse prognosis compared to wild‐type tumours 121, 123 |