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Publication : Loss of CEACAM1 in endothelial cells causes hepatic fibrosis.

First Author  Muturi HT Year  2023
Journal  Metabolism Volume  144
Pages  155562 PubMed ID  37088122
Mgi Jnum  J:335460 Mgi Id  MGI:7470567
Doi  10.1016/j.metabol.2023.155562 Citation  Muturi HT, et al. (2023) Loss of CEACAM1 in endothelial cells causes hepatic fibrosis. Metabolism 144:155562
abstractText  OBJECTIVES: Hepatocytic CEACAM1 plays a critical role in NASH pathogenesis, as bolstered by the development of insulin resistance, visceral obesity, steatohepatitis and fibrosis in mice with global Ceacam1 (Cc1) deletion. In contrast, VECadCre+Cc1(fl/fl) mice with endothelial loss of Cc1 manifested insulin sensitivity with no visceral obesity despite elevated NF-kappaB signaling and increased systemic inflammation. We herein investigated whether VECadCre+Cc1(fl/fl) male mice develop hepatic fibrosis and whether this is mediated by increased production of endothelin1 (ET1), a transcriptional NF-kappaB target. METHODS: VECadCre+Et1.Cc1(fl/fl) mice with combined endothelial loss of Cc1/Et1 genes were generated. Histological and immunohistochemical analyses were conducted on their livers and on liver tissue biopsies from adult patients undergoing bariatric surgery or from patients with NASH diagnosis receiving liver transplant. RESULTS: Hepatic fibrosis and inflammatory infiltration developed in VECadCre+Cc1(fl/fl) liver parenchyma. This was preceded by increased ET1 production and reversed with combined endothelial loss of Et1. Conditioned media from VECadCre+Cc1(fl/fl), but not VECadCre+Et1.Cc1(fl/fl) primary liver endothelial cells activated wild-type hepatic stellate cells; a process inhibited by bosentan, an ET(A)R/ET(B)R dual antagonist. Consistently, immunohistochemical analysis of liver biopsies from patients with NASH showed a decline in endothelial CEACAM1 in parallel with increased plasma endothelin1 levels and progression of hepatic fibrosis stage. CONCLUSIONS: The data demonstrated that endothelial CEACAM1 plays a key role in preventing hepatic fibrogenesis by reducing autocrine endothelin1 production.
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