Correlation of MRI signal characteristics of intracranial melanoma metastases with BRAF mutation status

BRAF V600 mutations (BRAF mut ) are associated with more pigmentation in primary melanomas, but data on melanin content of metastases are limited. This study compares signal characteristics of BRAF mut and BRAF-wildtype (BRAF wt ) intracranial melanoma metastases (IMM). MRI brain examinations at first diagnosis of IMM were identified, all performed at 3-Tesla including 1 mm volumetric pre- and postcontrast T1-weighted imaging and susceptibility-weighted imaging (SWI). Individual metastases were assessed by a neuroradiologist, stratified by size (≥10 mm, ‘larger’, vs. 2–9 mm, ‘small’; up to 10 per group); presence of intrinsic T1-hyperintensity (T1H) and, if present, whether confidently attributable to melanin as opposed to haemorrhage; evidence of haemorrhage; presence of central necrosis. A total of 267 IMM in 73 patients were assessed (87 larger IMM, 180 small). The proportion of larger IMM was similar in both groups (31% BRAF mut and 36% BRAF wt ). In small IMM, MRI evidence of melanin was more common in BRAF mut patients (42% vs. 26%; P = 0.038). Haemorrhage was more common in larger IMM (51%, vs. 20% of small IMM; P < 0.0001), but did not differ based on BRAF status. Central necrosis was more common in larger IMM (44% vs. 7%; P < 0.0001) and in BRAF mut IMM (23% vs. 11%; P = 0.011). In the BRAF mut cohort, central necrosis was more common in patients without previous anti-BRAF therapy (33% vs. 7%; P = 0.0001). T1H attributable to melanin is only slightly more common in BRAF mut IMM than BRAF wt . Higher rates of central necrosis in BRAF mut patients without previous anti-BRAF therapy suggest that anti-BRAF therapy may affect the patterns of IMM growth.