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Androgen receptor is a determinant of melanoma targeted drug resistance

Anastasia Samarkina, Markus K. Youssef, Paola Ostano, Soumitra Ghosh, Min Ma, Beatrice Tassone, Tatiana Proust, Giovanna Chiorino, Mitchell P. Levesque, Sandro Goruppi, G. Paolo Dotto

2023Nature Communications35 citationsDOIOpen Access PDF

Abstract

Abstract Melanoma provides a primary benchmark for targeted drug therapy. Most melanomas with BRAF V600 mutations regress in response to BRAF/MEK inhibitors (BRAFi/MEKi). However, nearly all relapse within the first two years, and there is a connection between BRAFi/MEKi-resistance and poor response to immune checkpoint therapy. We reported that androgen receptor (AR) activity is required for melanoma cell proliferation and tumorigenesis. We show here that AR expression is markedly increased in BRAFi-resistant melanoma cells, and in sensitive cells soon after BRAFi exposure. Increased AR expression is sufficient to render melanoma cells BRAFi-resistant, eliciting transcriptional changes of BRAFi-resistant subpopulations, including elevated EGFR and SERPINE1 expression, of likely clinical significance. Inhibition of AR expression or activity blunts changes in gene expression and suppresses proliferation and tumorigenesis of BRAFi-resistant melanoma cells, promoting clusters of CD8 + T cells infiltration and cancer cells killing. Our findings point to targeting AR as possible co-therapeutical approach in melanoma treatment.

Topics & Concepts

Cancer researchMelanomaAndrogen receptorCarcinogenesisGene knockdownMedicineDrug resistanceImmune checkpointCell growthTrametinibCytotoxic T cellCancerBiologyCell cultureImmunotherapySignal transductionProstate cancerInternal medicineMAPK/ERK pathwayCell biologyGeneticsBiochemistryMicrobiologyIn vitroMelanoma and MAPK PathwaysImmunotherapy and Immune ResponsesCAR-T cell therapy research
Androgen receptor is a determinant of melanoma targeted drug resistance | Litcius