Table 1.
Potential cutaneous melanoma biomarkers detected by immunohistochemical analysis of tissue microarrays
| Biomarker | Observation | Ref. |
| Hsp90 | Increased expression in melanomas compared with nevi and in metastatic compared with primary tumours. Correlation with tumour thickness and higher Clark level. No association seen between high expression and survival in the subsets of patients with primary or metastatic tumours. | [23] |
| RGS1 | Correlation with increased tumour thickness, mitotic rate and vascular involvement; reduced RFS and DSS. | [24] |
| Osteopontin | Correlation with increased tumour thickness, higher Clark level, mitotic index; reduced RFS and DSS; predictive of SLN metastasis and SLN burden. | [25] |
| HER3 | Correlation with increased cell proliferation, tumour progression; reduced survival. | [26] |
| ING4 | Reduced levels associated with melanoma thickness, ulceration and poor DSS and OS. | [27] |
| ING3 | Reduced nuclear expression associated with poor DSS; an independent prognostic factor to predict patient outcome. | [28] |
| NCOA3 | Increased levels predictive of SLN metastasis and associated with poor RFS and DSS. | [29] |
| MCM4 | Increased levels associated with poor DFS and OS. | [5] |
| MCM6 | Increased levels associated with poor DFS and OS. | [5] |
DFS, disease-free survival; DSS, disease-specific survival; IHC, immunohistochemistry; OS, overall survival; RFS, relapse-free survival; SLN, sentinel lymph node.