Publication | Open Access
Altered BAF occupancy and transcription factor dynamics in PBAF-deficient melanoma
41
Citations
85
References
2022
Year
GeneticsPathologyCancer BiologyChromatin AccessibilityEpigeneticsTumor BiologyMelanoma CellsTranscriptional RegulationArid2 DeficiencyCell SignalingTranscription FactorsCancer ResearchMelanomaTranscription Factor DynamicsGene ExpressionFunctional GenomicsCell BiologyTumor MicroenvironmentChromatin FunctionChromatinChromatin RemodelingNatural SciencesCancer GenomicsTumor SuppressorSystems BiologyMedicine
ARID2 is the most recurrently mutated SWI/SNF complex member in melanoma; however, its tumor-suppressive mechanisms in the context of the chromatin landscape remain to be elucidated. Here, we model ARID2 deficiency in melanoma cells, which results in defective PBAF complex assembly with a concomitant genomic redistribution of the BAF complex. Upon ARID2 depletion, a subset of PBAF and shared BAF-PBAF-occupied regions displays diminished chromatin accessibility and associated gene expression, while BAF-occupied enhancers gain chromatin accessibility and expression of genes linked to the process of invasion. As a function of altered accessibility, the genomic occupancy of melanoma-relevant transcription factors is affected and significantly correlates with the observed transcriptional changes. We further demonstrate that ARID2-deficient cells acquire the ability to colonize distal organs in multiple animal models. Taken together, our results reveal a role for ARID2 in mediating BAF and PBAF subcomplex chromatin dynamics with consequences for melanoma metastasis.
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