- In, Gino K;
- Ribeiro, Jennifer R;
- Yin, Jun;
- Xiu, Joanne;
- Bustos, Matias A;
- Ito, Fumito;
- Chow, Frances;
- Zada, Gabriel;
- Hwang, Lindsay;
- Salama, April KS;
- Park, Soo J;
- Moser, Justin C;
- Darabi, Sourat;
- Domingo-Musibay, Evidio;
- Ascierto, Maria L;
- Margolin, Kim;
- Lutzky, Jose;
- Gibney, Geoffrey T;
- Atkins, Michael B;
- Izar, Benjamin;
- Hoon, Dave SB;
- VanderWalde, Ari M
Melanoma brain metastases (MBM) are clinically challenging to treat and exhibit variable responses to immune checkpoint therapies. Prior research suggests that MBM exhibit poor tumor immune responses and are enriched in oxidative phosphorylation. Here, we report results from a multi-omic analysis of a large, real-world melanoma cohort. MBM exhibited lower interferon-gamma (IFNγ) scores and T cell-inflamed scores compared to primary cutaneous melanoma (PCM) or extracranial metastases (ECM), which was independent of tumor mutational burden. Among MBM, there were fewer computationally inferred immune cell infiltrates, which correlated with lower TNF and IL12B mRNA levels. Ingenuity pathway analysis (IPA) revealed suppression of inflammatory responses and dendritic cell maturation pathways. MBM also demonstrated a higher frequency of pathogenic PTEN mutations and angiogenic signaling. Oxidative phosphorylation (OXPHOS) was enriched in MBM and negatively correlated with NK cell and B cell-associated transcriptomic signatures. Modulating metabolic or angiogenic pathways in MBM may improve responses to immunotherapy in this difficult-to-treat patient subset.