Endogenous glucocorticoids are required for normal macrophage activation and gastric Helicobacter pylori immunity [RNA-seq]

Glucocorticoids are steroid hormones well-known for their potent anti-inflammatory effects. However, their immunomodulatory properties are multifaceted. Increasing evidence suggests that glucocorticoid signaling promotes effective immunity and that disruption of glucocorticoid signaling impairs immune function. In this study, we conditionally deleted the glucocorticoid receptor (GR) in the myeloid lineage using theLysM-Credriver (myGRKO). We examined the impact on macrophage activation and gastric immune responses toHelicobacter pylori, the best-known risk factor of gastric cancer. Our results indicate that compared to WT, GRKO macrophages exhibited higher expression of proinflammatory genes in steroid-free conditions. However, when challenged in vivo, GRKO macrophages exhibited aberrant chromatin landscapes and impaired proinflammatory gene expression profiles. Moreover, gastric colonization withHelicobacterrevealed impaired gastric immune responses and reduced T cell recruitment in myGRKO mice. As a result, myGRKO mice were protected from atrophic gastritis and pyloric metaplasia development. These results demonstrate a dual role for glucocorticoid signaling in preparing macrophages to respond to bacterial infection but limiting their pathogenic activation. In addition, our results support that macrophages are critical for gastric anti-Helicobacterimmunity. Overall design: RNAseq of freshly isolated thioglycollate-induced peritoneal macrophages isolated from vehicle-treated WT mice, vehicle-treated mice with Nr3c1 deletion with the Lysm Cre driver or the same genotypes treated in vivo for 3 hours with Helicobacter pylori. There are 4 replicates per group.