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Publication : RelB promotes liver fibrosis via inducing the release of injury-associated inflammatory cytokines.

First Author  Zhou D Year  2020
Journal  J Cell Mol Med Volume  24
Issue  11 Pages  6008-6014
PubMed ID  32306539 Mgi Jnum  J:305745
Mgi Id  MGI:6705317 Doi  10.1111/jcmm.15108
Citation  Zhou D, et al. (2020) RelB promotes liver fibrosis via inducing the release of injury-associated inflammatory cytokines. J Cell Mol Med 24(11):6008-6014
abstractText  Liver fibrosis is a serious chronic disease that developed by a coordinated interplay of many cell types, but the underlying signal transduction in individual cell type remains to be characterized. Nuclear factor-kappaB (NF-kappaB) is a widely accepted central player in the development of hepatic fibrosis. However, the precise role of each member of NF-kappaB in different cell type is unclear. Here, we generated a mouse model (Relb(Deltahep) ) with hepatocyte-specific deletion of RelB, a member of NF-kappaB family. Relb(Deltahep) mice born normally and appear normal without obvious abnormality. However, in the CCl4-induced liver fibrosis, Relb(Deltahep) mice developed less severe disease compared with wide-type (WT) mice. The denaturation and necrosis of hepatocytes as well as the formation of false lobules in Relb(Deltahep) mice were significantly reduced compared with WT mice. The production of alpha-SMA and the level of collagen I and Collagen III were greatly reduced in Relb(Deltahep) mice comparing with WT mice. Furthermore, in patients with liver fibrosis, RelB is up-regulated along with the stage of diseases. Consistently, CCl4 treatment could up-regulate the expression of RelB as well as inflammatory cytokines such as IL-6 and TGF-beta1 in hepatoma cell as well as in WT mice. Knockdown the expression of RelB in hepatoma cells greatly reduced the expression of CCl4-induced inflammatory cytokines. In summary, we provide the genetic evidence to demonstrate the critical and hepatocellular role of RelB in liver fibrosis. RelB is an important transcription factor to drive the expression of inflammatory cytokines in the initiation phase of injury.
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