Publication | Open Access
The ETS Family Transcription Factors Etv5 and PU.1 Function in Parallel To Promote Th9 Cell Development
48
Citations
38
References
2016
Year
Inflammatory Lung DiseaseLung InflammationGeneticsImmunologyImmune RegulationMolecular GeneticsCd4 T Cell ResponsesInnate ImmunityImmune SystemImmune DysregulationInflammationIl-9-secreting Th9 SubsetTranscriptional RegulationCd4 Th CellsImmunopathologyTh9 Cell DevelopmentAutoimmune DiseaseAllergyTh9 CellsAutoimmunityT Cell ImmunityGene ExpressionCell BiologyTranscription RegulationPu.1 FunctionImmune Cell DevelopmentGene RegulationDevelopmental ImmunologyTranscription FactorsMedicineCell Development
The IL-9-secreting Th9 subset of CD4 Th cells develop in response to an environment containing IL-4 and TGF-β, promoting allergic disease, autoimmunity, and resistance to pathogens. We previously identified a requirement for the ETS family transcription factor PU.1 in Th9 development. In this report, we demonstrate that the ETS transcription factor ETS variant 5 (ETV5) promotes IL-9 production in Th9 cells by binding and recruiting histone acetyltransferases to the Il9 locus at sites distinct from PU.1. In cells that are deficient in both PU.1 and ETV5 there is lower IL-9 production than in cells lacking either factor alone. In vivo loss of PU.1 and ETV5 in T cells results in distinct effects on allergic inflammation in the lung, suggesting that these factors function in parallel. Together, these data define a role for ETV5 in Th9 development and extend the paradigm of related transcription factors having complementary functions during differentiation.
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