Protein kinase a‐dependent pSer675‐β‐catenin, a novel signaling defect in a mouse model of congenital hepatic fibrosis. Issue 5 (30th September 2013)
- Record Type:
- Journal Article
- Title:
- Protein kinase a‐dependent pSer675‐β‐catenin, a novel signaling defect in a mouse model of congenital hepatic fibrosis. Issue 5 (30th September 2013)
- Main Title:
- Protein kinase a‐dependent pSer675‐β‐catenin, a novel signaling defect in a mouse model of congenital hepatic fibrosis
- Authors:
- Spirli, Carlo
Locatelli, Luigi
Morell, Carola M.
Fiorotto, Romina
Morton, Stuart D.
Cadamuro, Massimiliano
Fabris, Luca
Strazzabosco, Mario - Abstract:
- Abstract : Genetically determined loss of fibrocystin function causes congenital hepatic fibrosis (CHF), Caroli disease (CD), and autosomal recessive polycystic kidney disease (ARPKD). Cystic dysplasia of the intrahepatic bile ducts and progressive portal fibrosis characterize liver pathology in CHF/CD. At a cellular level, several functional morphological and signaling changes have been reported including increased levels of 3′‐5′‐cyclic adenosine monophosphate (cAMP). In this study we addressed the relationships between increased cAMP and β‐catenin. In cholangiocytes isolated and cultured from Pkhd1 del4/del4 mice, stimulation of cAMP/PKA signaling (forskolin 10 μM) stimulated Ser 675 ‐phosphorylation of β‐catenin, its nuclear localization, and its transcriptional activity (western blot and TOP flash assay, respectively) along with a down‐regulation of E‐cadherin expression (immunocytochemistry and western blot); these changes were inhibited by the PKA blocker, PKI (1 μM). The Rho‐GTPase, Rac‐1, was also significantly activated by cAMP in Pkhd1 del4/del4 cholangiocytes. Rac‐1 inhibition blocked cAMP‐dependent nuclear translocation and transcriptional activity of pSer 675 ‐β‐catenin. Cell migration (Boyden chambers) was significantly higher in cholangiocytes obtained from Pkhd1 del4/del4 and was inhibited by: (1) PKI, (2) silencing β‐catenin (siRNA), and (3) the Rac‐1 inhibitor NSC 23766. Conclusion : These data show that in fibrocystin‐defective cholangiocytes, cAMP/PKAAbstract : Genetically determined loss of fibrocystin function causes congenital hepatic fibrosis (CHF), Caroli disease (CD), and autosomal recessive polycystic kidney disease (ARPKD). Cystic dysplasia of the intrahepatic bile ducts and progressive portal fibrosis characterize liver pathology in CHF/CD. At a cellular level, several functional morphological and signaling changes have been reported including increased levels of 3′‐5′‐cyclic adenosine monophosphate (cAMP). In this study we addressed the relationships between increased cAMP and β‐catenin. In cholangiocytes isolated and cultured from Pkhd1 del4/del4 mice, stimulation of cAMP/PKA signaling (forskolin 10 μM) stimulated Ser 675 ‐phosphorylation of β‐catenin, its nuclear localization, and its transcriptional activity (western blot and TOP flash assay, respectively) along with a down‐regulation of E‐cadherin expression (immunocytochemistry and western blot); these changes were inhibited by the PKA blocker, PKI (1 μM). The Rho‐GTPase, Rac‐1, was also significantly activated by cAMP in Pkhd1 del4/del4 cholangiocytes. Rac‐1 inhibition blocked cAMP‐dependent nuclear translocation and transcriptional activity of pSer 675 ‐β‐catenin. Cell migration (Boyden chambers) was significantly higher in cholangiocytes obtained from Pkhd1 del4/del4 and was inhibited by: (1) PKI, (2) silencing β‐catenin (siRNA), and (3) the Rac‐1 inhibitor NSC 23766. Conclusion : These data show that in fibrocystin‐defective cholangiocytes, cAMP/PKA signaling stimulates pSer 675 ‐phosphorylation of β‐catenin and Rac‐1 activity. In the presence of activated Rac‐1, pSer 675 ‐β‐catenin is translocated to the nucleus, becomes transcriptionally active, and is responsible for increased motility of Pkhd1 del4/del4 cholangiocytes. β‐Catenin‐dependent changes in cell motility may be central to the pathogenesis of the disease and represent a potential therapeutic target. (Hepatology 2013;58:1713–1723) … (more)
- Is Part Of:
- Hepatology. Volume 58:Issue 5(2013:Nov.)
- Journal:
- Hepatology
- Issue:
- Volume 58:Issue 5(2013:Nov.)
- Issue Display:
- Volume 58, Issue 5 (2013)
- Year:
- 2013
- Volume:
- 58
- Issue:
- 5
- Issue Sort Value:
- 2013-0058-0005-0000
- Page Start:
- 1713
- Page End:
- 1723
- Publication Date:
- 2013-09-30
- Subjects:
- Heart -- Diseases -- Nursing -- Periodicals
Lungs -- Diseases -- Nursing -- Periodicals
Intensive care nursing -- Periodicals
Foie -- Maladies -- Périodiques
616.362 - Journal URLs:
- http://onlinelibrary.wiley.com/journal/10.1002/(ISSN)1527-3350 ↗
http://onlinelibrary.wiley.com/ ↗ - DOI:
- 10.1002/hep.26554 ↗
- Languages:
- English
- ISSNs:
- 0270-9139
- Deposit Type:
- Legaldeposit
- View Content:
- Available online (eLD content is only available in our Reading Rooms) ↗
- Physical Locations:
- British Library DSC - 4295.836000
British Library DSC - BLDSS-3PM
British Library HMNTS - ELD Digital store - Ingest File:
- 8812.xml