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Publication : CITED2 limits pathogenic inflammatory gene programs in myeloid cells.

First Author  Pong Ng H Year  2020
Journal  FASEB J Volume  34
Issue  9 Pages  12100-12113
PubMed ID  32697413 Mgi Jnum  J:304244
Mgi Id  MGI:6694452 Doi  10.1096/fj.202000864R
Citation  Pong Ng H, et al. (2020) CITED2 limits pathogenic inflammatory gene programs in myeloid cells. FASEB J 34(9):12100-12113
abstractText  Monocyte-derived macrophages are the major innate immune cells that provide the first line of cellular defense against infections or injuries. These recruited macrophages at the site of inflammation are exposed to a broad range of cytokines that categorically incite a robust pro-inflammatory response. However, macrophage pro-inflammatory activation must be under exquisite control to avert unbridled inflammation. Thus, endogenous mechanisms must exist that rigorously preserve macrophage quiescence and yet, allow nimble pro-inflammatory macrophage response with precise spatiotemporal control. Herein, we identify the CBP/p300-interacting transactivator with glutamic acid/aspartic acid-rich carboxyl-terminal domain 2 (CITED2) as a critical intrinsic negative regulator of inflammation, which broadly attenuates pro-inflammatory gene programs in macrophages. Our in vivo studies revealed that myeloid-CITED2 deficiency significantly heightened macrophages and neutrophils recruitment to the site of inflammation. Our integrated transcriptomics and gene set enrichment analysis (GSEA) studies uncovered that CITED2 deficiency broadly enhances NFkappaB targets, IFNgamma/IFNalpha responses, and inflammatory response gene expression in macrophages. Using complementary gain- and loss-of-function studies, we observed that CITED2 overexpression attenuate and CITED2 deficiency elevate LPS-induced NFkappaB transcriptional activity and NFkappaB-p65 recruitment to target gene promoter in macrophages. More importantly, blockade of NFkappaB signaling completely reversed elevated pro-inflammatory gene expression in macrophages. Collectively, our findings show that CITED2 restrains NFkappaB activation and curtails broad pro-inflammatory gene programs in myeloid cells.
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