Abstract

Cystic Fibrosis (CF) is a common and clinically severe genetic disease, caused by mutations in CFTR, a membrane protein that mediates chloride and fluid secretion in a number of secretory epithelia, including the biliary tree. Cystic Fibrosis liver disease (CFLD) is a chronic cholangiopathy that can eventually evolve into sclerosing cholangitis and focal biliary cirrhosis. The pathogenesis of this condition is not well understood and treatment is limited to the administration of choleretic bile acids, or in selected cases, liver transplantation. CFLD has been classically considered a consequence of the impaired bile secretion caused by the defective CFTR channel function. However, while biliary secretion is universally reduced in CF, the spontaneous development of CFLD is less frequent, suggesting that genetic and/or acquired factors are at play. Our previous studies suggested that reduced tolerance of the biliary innate immune system to endotoxins plays a major pathogenetic role in CFLD. We showed that cholangiocytes isolated from Cftr-KO mice have higher NF-?B activity and secrete a larger amount of inflammatory cytokines, when exposed to the TLR4-ligand LPS. We have also demonstrated that in CF-defective cholangiocytes, TLR4 is activated by the unrestrained function of Src family kinases (SFK), a consequence of defective CFTR. This mechanism is present also in cholangiocytes derived from human iPSC homozygous for the ?F508 mutation. In addition, novel exciting preliminary data show that the gut microbiota in CFTR-KO mice is already different from WT littermates at birth and it is skewed towards the prevalence of a more pro-inflammatory flora. In this application we will test the hypothesis that CFLD may result from the combination of a genetic mutation affecting biliary epithelial innate immunity along with changes in microbiota composition and increased intestinal permeability. In particular, (1) we will use iPSC technology to dissect the impact of functionally different CFTR mutations on the mechanisms leading to a pro-inflammatory phenotype in human cholangiocytes and (2) we will study whether changes in the gut microbiota play a causal role in the development of liver disease in mouse models of CF. Our study will discover novel aspects of secretory epithelia physiology and innate immunity and clarity if changes in the gut microbiota play a possible causal role in CFLD. These studies represent a paradigm-shift in the understanding of the pathogenesis of CFLD and imply that treatment for CFLD should also control inflammation and the impact of the intestinal microbiota. The outcome of this project will lay the foundation for novel intervention strategies that will have an impact on the management of CFLD and other cholangiopathies. !

Public Health Relevance

Cystic Fibrosis liver disease (CFLD) negatively impacts the quality of life and survival of CF patients, and may require liver transplantation, however, the pathogenesis of this condition is not well understood. Our proposal will test the hypothesis that CFLD may result from the combination of a genetic mutation affecting biliary epithelial innate immunity along with changes in gut microbial composition and increased intestinal permeability. Using human cholangiocytes derived from induced pluripotent stem cells (iPSC) and microbiota studies in mice, we will propose novel intervention strategies that will have an impact on the management of CFLD.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Diabetes and Digestive and Kidney Diseases (NIDDK)
Type
Research Project (R01)
Project #
2R01DK096096-06A1
Application #
9685346
Study Section
Special Emphasis Panel (ZRG1)
Program Officer
Sherker, Averell H
Project Start
2013-05-01
Project End
2023-07-31
Budget Start
2018-09-22
Budget End
2019-07-31
Support Year
6
Fiscal Year
2018
Total Cost
Indirect Cost

  Institution

Name
Yale University
Department
Internal Medicine/Medicine
Type
Schools of Medicine
DUNS #
043207562
City
New Haven
State
CT
Country
United States
Zip Code

  Publications

Strazzabosco, Mario; Fiorotto, Romina; Cadamuro, Massimiliano et al. (2018) Pathophysiologic implications of innate immunity and autoinflammation in the biliary epithelium. Biochim Biophys Acta Mol Basis Dis 1864:1374-1379
Mariotti, Valeria; Strazzabosco, Mario; Fabris, Luca et al. (2018) Animal models of biliary injury and altered bile acid metabolism. Biochim Biophys Acta Mol Basis Dis 1864:1254-1261
Fiorotto, Romina; Amenduni, Mariangela; Mariotti, Valeria et al. (2018) Src kinase inhibition reduces inflammatory and cytoskeletal changes in ?F508 human cholangiocytes and improves cystic fibrosis transmembrane conductance regulator correctors efficacy. Hepatology 67:972-988
Morell, Carola M; Fiorotto, Romina; Meroni, Marica et al. (2017) Notch signaling and progenitor/ductular reaction in steatohepatitis. PLoS One 12:e0187384
De Carlis, Luciano; Di Sandro, Stefano; Centonze, Leonardo et al. (2016) Liver-allocation policies for patients affected by HCC in Europe. Curr Transplant Rep 3:313-318
Fiorotto, Romina; Villani, Ambra; Kourtidis, Antonis et al. (2016) The cystic fibrosis transmembrane conductance regulator controls biliary epithelial inflammation and permeability by regulating Src tyrosine kinase activity. Hepatology 64:2118-2134
Scirpo, Roberto; Fiorotto, Romina; Villani, Ambra et al. (2015) Stimulation of nuclear receptor peroxisome proliferator-activated receptor-? limits NF-?B-dependent inflammation in mouse cystic fibrosis biliary epithelium. Hepatology 62:1551-62
Bonato, Giulia; Cristoferi, Laura; Strazzabosco, Mario et al. (2015) Malignancies in Primary Sclerosing Cholangitis--A Continuing Threat. Dig Dis 33 Suppl 2:140-8
Fouassier, Laura; Fiorotto, Romina (2015) Ezrin finds its groove in cholangiocytes. Hepatology 61:1467-70
Fickert, Peter; Pollheimer, Marion J; Beuers, Ulrich et al. (2014) Characterization of animal models for primary sclerosing cholangitis (PSC). J Hepatol 60:1290-303