Litcius/Paper detail

Toll-like receptor 4 signaling activates ERG function in prostate cancer and provides a therapeutic target

Benjamin M. Greulich, Joshua P. Plotnik, Travis J. Jerde, Peter C. Hollenhorst

2021NAR Cancer17 citationsDOIOpen Access PDF

Abstract

gene fusion and subsequent overexpression of the ERG transcription factor occurs in ∼50% of prostate tumors, making it the most common abnormality of the prostate cancer genome. While ERG has been shown to drive tumor progression and cancer-related phenotypes, as a transcription factor it is difficult to target therapeutically. Using a genetic screen, we identified the toll-like receptor 4 (TLR4) signaling pathway as important for ERG function in prostate cells. Our data confirm previous reports that ERG can transcriptionally activate TLR4 gene expression; however, using a constitutively active ERG mutant, we demonstrate that the critical function of TLR4 signaling is upstream, promoting ERG phosphorylation at serine 96 and ERG transcriptional activation. The TLR4 inhibitor, TAK-242, attenuated ERG-mediated migration, clonogenic survival, target gene activation and tumor growth. Together these data indicate a mechanistic basis for inhibition of TLR4 signaling as a treatment for ERG-positive prostate cancer.

Topics & Concepts

ErgProstate cancerTMPRSS2Cancer researchETS transcription factor familyTranscription factorBiologySignal transductionTLR4ChromoplexyProstateFusion geneCancerGeneMedicineCell biologyInternal medicineGeneticsPCA3NeuroscienceCoronavirus disease 2019 (COVID-19)Infectious disease (medical specialty)DiseaseRetinaProstate Cancer Treatment and ResearchNF-κB Signaling Pathwaysinterferon and immune responses