Aggf1 attenuates hepatic inflammation and activation of hepatic
stellate cells by repressing Ccl2 transcription
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Graphical Abstract
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Abstract
Liver injury represents a continuum of pathophysiological processes involving a complex interplay between
hepatocytes, macrophages, and hepatic stellate cells. The mechanism whereby these intercellular interactions
contribute to liver injury and fibrosis is not completely understood. We report here that angiogenic factor with G patch
and FHA domains 1 (Aggf1) was downregulated in the livers of cirrhotic patients compared to healthy controls and in
primary hepatocytes in response to carbon tetrachloride (CCl4) stimulation. Overexpression of Aggf1 attenuated
macrophage chemotaxis. Aggf1 interacted with NF-κB to block its binding to the Ccl2 gene promoter and repressed
Ccl2 transcription in hepatocytes. Macrophages cultured in the conditioned media collected from Aggf1-
overexpressing hepatocytes antagonized HSC activation. Taken together, our data illustrate a novel role for Aggf1 in
regulating hepatic inflammation and provide insights on the development of interventional strategies against cirrhosis.
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