Litcius/Paper detail

MEF2A suppresses stress responses that trigger DDX41-dependent IFN production

Julian R. Smith, Jack W. Dowling, Matthew I. McFadden, Andrew Karp, Johannes Schwerk, Joshua J. Woodward, Ram Savan, Adriana Forero

2023Cell Reports22 citationsDOIOpen Access PDF

Abstract

Cellular stress in the form of disrupted transcription, loss of organelle integrity, or damage to nucleic acids can elicit inflammatory responses by activating signaling cascades canonically tasked with controlling pathogen infections. These stressors must be kept in check to prevent unscheduled activation of interferon, which contributes to autoinflammation. This study examines the role of the transcription factor myocyte enhancing factor 2A (MEF2A) in setting the threshold of transcriptional stress responses to prevent R-loop accumulation. Increases in R-loops lead to the induction of interferon and inflammatory responses in a DEAD-box helicase 41 (DDX41)-, cyclic GMP-AMP synthase (cGAS)-, and stimulator of interferon genes (STING)-dependent manner. The loss of MEF2A results in the activation of ATM and RAD3-related (ATR) kinase, which is also necessary for the activation of STING. This study identifies the role of MEF2A in sustaining transcriptional homeostasis and highlights the role of ATR in positively regulating R-loop-associated inflammatory responses.

Topics & Concepts

Stimulator of interferon genesTranscription factorInterferonCell biologyKinaseStingBiologySignal transductionTranscription (linguistics)Innate immune systemImmunologyImmune systemGeneGeneticsPhysicsThermodynamicsLinguisticsPhilosophyinterferon and immune responsesRNA regulation and diseaseInflammasome and immune disorders