Melanoma plasticity is controlled by a TRIM28-JUNB mediated switch

Abstract: The introduction of immune checkpoint blockade has revolutionized the treatment of metastatic melanoma1. However, 40-60% of patients with metastatic melanoma do not respond to immune checkpoint blockade, and a significant fraction of patients acquire resistance to treatment2,3. This resilience and aggressiveness of melanoma tumors is partly due to their ability to switch between invasive and proliferative states4,5. The transition between phenotypic states indicates that phenotype switching occurs through reve… Show more

“…Another AP-1 family member, Fra1 ( FOSL1 ), downregulates MITF through its transcriptional target, the chromatin modifier HMGA1, and induces the expression of AXL, driving melanoma cells to the MITF low /AXL high state ( 53 ). Notably, while c-Jun and Fra1 promote the melanoma switch to the invasive phenotype, other AP-1 transcription factors, such as Fra2 ( 63 ) and perhaps JunB ( 62 ) inhibit this switch. These studies indicate that AP-1 mediates plasticity by the differing composition of its subunits, similar to the aforementioned ZEB2/ZEB1 and LEF1/TCF4 switch.…”

Melanoma Plasticity: Promoter of Metastasis and Resistance to Therapy

“…Another AP-1 family member, Fra1 ( FOSL1 ), downregulates MITF through its transcriptional target, the chromatin modifier HMGA1, and induces the expression of AXL, driving melanoma cells to the MITF low /AXL high state ( 53 ). Notably, while c-Jun and Fra1 promote the melanoma switch to the invasive phenotype, other AP-1 transcription factors, such as Fra2 ( 63 ) and perhaps JunB ( 62 ) inhibit this switch. These studies indicate that AP-1 mediates plasticity by the differing composition of its subunits, similar to the aforementioned ZEB2/ZEB1 and LEF1/TCF4 switch.…”

Melanoma Plasticity: Promoter of Metastasis and Resistance to Therapy