Publication date: Jun 23, 2025
While combination BRAF/MEK inhibition has improved survival in BRAF mutant melanoma, targeted therapies for BRAF melanoma remain limited. Microphthalmia transcription factor (MITF), a lineage-specific transcription factor that regulates melanocyte proliferation and melanin synthesis, represents a promising melanoma-specific drug target. In this study, we evaluated TT-012, a recently identified MITF dimerization specific inhibitor, and surprisingly found that most BRAF melanoma lines were resistant to TT-012 due to low MITF transcriptional activity and reduced dependency on MITF for proliferation. High-throughput drug screen identified tivozanib, an FDA-approved drug targeting VEGFR and other receptor tyrosine kinases (RTKs), which sensitized cells to TT-012. Mechanistically, tivozanib induced cell state transition from MITF to MITF state via VEGFR2 inhibition followed by NF-_705B pathway activation, restoring MITF transcriptional activity and growth dependency. The combination of tivozanib and TT-012 synergistically inhibited melanoma growth both in vitro and in vivo, underscoring its potential as a novel therapeutic strategy for BRAF melanoma.
| Concepts | Keywords |
|---|---|
| Drug | BRAF WT melanoma |
| Fda | cell state plasticity |
| Kinases | MITF |
| Melanoma | tivozanib |
| Wild | TT-012 |
| VEGFR2 |
Semantics
| Type | Source | Name |
|---|---|---|
| drug | DRUGBANK | Tivozanib |
| disease | MESH | melanoma |
| pathway | KEGG | Melanoma |
| disease | MESH | Microphthalmia |
| drug | DRUGBANK | L-Tyrosine |