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Loss of <scp>CEACAM1</scp> in hepatocytes causes hepatic fibrosis

Sobia Zaidi, Suman Asalla, Harrison T. Muturi, Lucia Russo, Raziyeh Abdolahipour, Getachew D. Belew, Maria Benitez Iglesias, Mary Feraudo, Lensay Leon, Enoch Kuo, Xiuli Liu, Sivarajan Kumarasamy, Hilda E. Ghadieh, Cara Gatto‐Weis, Ali Zarrinpar, Sergio Duarte, Sonia M. Najjar

2024European Journal of Clinical Investigation18 citationsDOIOpen Access PDF

Abstract

Abstract Background The role of insulin resistance in hepatic fibrosis in Metabolic dysfunction‐Associated SteatoHepatitis (MASH) remains unclear. Carcinoembryonic Antigen‐related Cell Adhesion Molecule1 protein (CEACAM1) promotes insulin clearance to maintain insulin sensitivity and repress de novo lipogenesis, as bolstered by the development of insulin resistance and steatohepatitis in AlbuminCre + Cc1 fl/fl mice with liver‐specific mouse gene encoding CEACAM1 protein (Ceacam1) deletion. We herein investigated whether these mice also developed hepatic fibrosis and whether hepatic CEACAM1 is reduced in patients with MASH at different fibrosis stages. Methods AlbuminCre + Cc1 fl/fl mice were fed a regular or a high‐fat diet before their insulin metabolism and action were assessed during IPGTT, and their livers excised for histochemical, immunohistochemical and Western blot analysis. Sirius red staining was used to assess fibrosis, and media transfer was employed to examine whether mutant hepatocytes activated hepatic stellate cells (HSCs). Hepatic CEACAM1 protein levels in patients with varying disease stages were assessed by ELISA. Results Hepatocytic deletion of Ceacam1 caused hyperinsulinemia‐driven insulin resistance emanating from reduced hepatic insulin clearance. AlbuminCre + Cc1 fl/fl livers showed inflammation, fibrosis and hepatic injury, with more advanced bridging and chicken‐wire hepatic fibrosis under high‐fat conditions. Media transferred from hepatocytes isolated from mutant mice activated control HSCs, likely owing to their elevated endothelin1 content. Interestingly, hepatic CEACAM1 levels were lower in the livers of patients with MASH and declined gradually with advanced fibrosis stage. Conclusions Hepatic CEACAM1 levels declined with progression of MASH in humans. The phenotype of AlbuminCre + Cc1 fl/fl mice assigned a key role to CEACAM1 loss from hepatocytes in hepatic fibrosis independently of other liver cells.

Topics & Concepts

FibrosisHepatic fibrosisMedicineCell biologyBiologyCancer researchInternal medicineLiver physiology and pathologyRadiopharmaceutical Chemistry and ApplicationsOrgan Transplantation Techniques and Outcomes