Abstract B15: Comprehensive cistromic characterization of SOX10, a lineage-specific genetic dependency in melanoma, via the integration of functional genomic approaches

Melanoma accounts for less than 5% of skin cancers, but a majority of skin cancer deaths. Genomic studies and drug discovery programs have led to the development of targeted therapies, including BRAF and MEK inhibitors, but the inevitable resistance to these targeted agents necessitates a greater understanding of melanoma biology and genetics. By integrating genome-wide functional genomic and transcriptomic data, we have identified SOX10 as a lineage-specific genetic dependency in melanoma independent of BRAF or NRAS mutation status. Subsequent analyses indicate that SOX10 dependency is highly correlated with SOX10 gene expression and functional in vitro experiments have confirmed the role of SOX10 in the proliferation and growth of melanoma cell lines regardless of their sensitivity to MAPK pathway inhibitors. Chromatin immunoprecipitation of endogenous SOX10 followed by sequencing (SOX10 ChIP-seq) combined with transcriptomic profiling (RNA-seq) following SOX10 depletion by shRNA in a panel of melanoma cell lines determined the SOX10 cistrome, the set of SOX10 target genes across the melanoma genome. Integration of the SOX10 cistrome with genetic dependency data may lead to novel therapeutic approaches in melanoma.Citation Format: Terence Wong, Cory Johannessen, Jingyu Fan, Henry Long, Shirley Liu, Levi Garraway. Comprehensive cistromic characterization of SOX10, a lineage-specific genetic dependency in melanoma, via the integration of functional genomic approaches [abstrac...
Source: Molecular Cancer Therapeutics - Category: Cancer & Oncology Authors: Tags: Finding Synthetic Lethal Interactions through Functional Genomics: Poster Presentations - Proffered Abstracts Source Type: research