Liver fibrosis is a strong predictor of long-term mortality in patients with non-alcoholic fatty liver disease. The mechanisms underlying the progression from the comparatively benign fatty liver state to advanced non-alcoholic steatohepatitis and liver fibrosis are incompletely understood. “Understanding the mechanism by which this condition becomes life threatening is key in our quest for the discovery of therapeutic solutions and preventative measures,” said Stephan Herzig.
Loss of identity results in dysfunction
The researchers used comparative genomics to analyze mechanisms that control the development and specialized functions of the most abundant cell type in the liver, the hepatocyte. “Our results demonstrated that during progression to non-alcoholic steatohepatitis, hepatocytes suffer from partial identity loss, they are re-programmed,” explained Anne Loft, first co-author of the article.The hepatocyte reprogramming is tightly controlled by a network of proteins acting as molecular switches, so-called ‘transcription factors’. Their activity results in the dysfunction of hepatocytes. The network of transcription factors that controls this process also plays a role in fibrosis progression. “These findings are important because they unravel the cellular mechanisms underlying non-alcoholic steatohepatitis. Knowing about the role of the protein networks and the identity loss of hepatocytes gives us potential intervention targets for the development of effective therapies” says Ana Alfaro, first co-author of the article.
Future work
Based on these findings, it will now be possible to develop novel approaches to effectively target certain nodes in the protein network to prevent disease progression or even revert existing fibrosis, something that is still not possible to-date.About the people
Stephan Herzig is Director of the Helmholtz Diabetes Center at Helmholtz Zentrum München. He holds the Chair for Molecular Metabolic Control at the Technical University of Munich and an Honorary Chair at Heidelberg University. Anne Loft and Ana Alfaro are first co-authors of the study at Helmholtz Zentrum München. All are part of the German Center for Diabetes Research (DZD).helmholtz-muenchen.de