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Alexander, William B.; Wang, Wenjia; Hill, Margaret A.; O'Dell, Michael R.; Ruffolo, Luis I.; Guo, Bing; Jackson, Katherine M.; Ullman, Nicholas; Friedland, Scott C.; McCall, Matthew N.; Patel, Ankit; Figueroa-Guilliani, Nathania; Georger, Mary; Belt, Brian A.; Whitney-Miller, Christa L.; Linehan, David C.; Murphy, Patrick J.; Hezel, Aram F.

Smad4 restricts injury-provoked biliary proliferation and carcinogenesis

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  • Media type: E-Article
  • Title: Smad4 restricts injury-provoked biliary proliferation and carcinogenesis
  • Contributor: Alexander, William B.; Wang, Wenjia; Hill, Margaret A.; O'Dell, Michael R.; Ruffolo, Luis I.; Guo, Bing; Jackson, Katherine M.; Ullman, Nicholas; Friedland, Scott C.; McCall, Matthew N.; Patel, Ankit; Figueroa-Guilliani, Nathania; Georger, Mary; Belt, Brian A.; Whitney-Miller, Christa L.; Linehan, David C.; Murphy, Patrick J.; Hezel, Aram F.
  • imprint: The Company of Biologists, 2024
  • Published in: Disease Models & Mechanisms
  • Language: English
  • DOI: 10.1242/dmm.050358
  • ISSN: 1754-8403; 1754-8411
  • Keywords: General Biochemistry, Genetics and Molecular Biology ; Immunology and Microbiology (miscellaneous) ; Medicine (miscellaneous) ; Neuroscience (miscellaneous)
  • Origination:
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  • Description: <jats:title>ABSTRACT</jats:title> <jats:p>Cholangiocarcinoma (CCA) is a deadly and heterogeneous type of cancer characterized by a spectrum of epidemiologic associations as well as genetic and epigenetic alterations. We seek to understand how these features inter-relate in the earliest phase of cancer development and through the course of disease progression. For this, we studied murine models of liver injury integrating the most commonly occurring gene mutations of CCA – including Kras, Tp53, Arid1a and Smad4 – as well as murine hepatobiliary cancer models and derived primary cell lines based on these mutations. Among commonly mutated genes in CCA, we found that Smad4 functions uniquely to restrict reactive cholangiocyte expansion to liver injury through restraint of the proliferative response. Inactivation of Smad4 accelerates carcinogenesis, provoking pre-neoplastic biliary lesions and CCA development in an injury setting. Expression analyses of Smad4-perturbed reactive cholangiocytes and CCA lines demonstrated shared enriched pathways, including cell-cycle regulation, MYC signaling and oxidative phosphorylation, suggesting that Smad4 may act via these mechanisms to regulate cholangiocyte proliferation and progression to CCA. Overall, we showed that TGFβ/SMAD4 signaling serves as a critical barrier restraining cholangiocyte expansion and malignant transformation in states of biliary injury.</jats:p>
  • Access State: Open Access