Cellular and Molecular Gastroenterology and Hepatology (Jan 2018)

Uncovering a Predictive Molecular Signature for the Onset of NASH-Related Fibrosis in a Translational NASH Mouse Model

  • Arianne van Koppen,
  • Lars Verschuren,
  • Anita M. van den Hoek,
  • Joanne Verheij,
  • Martine C. Morrison,
  • Kelvin Li,
  • Hiroshi Nagabukuro,
  • Adalberto Costessi,
  • Martien P.M. Caspers,
  • Tim J. van den Broek,
  • John Sagartz,
  • Cornelis Kluft,
  • Carine Beysen,
  • Claire Emson,
  • Alain J. van Gool,
  • Roel Goldschmeding,
  • Reinout Stoop,
  • Ivana Bobeldijk-Pastorova,
  • Scott M. Turner,
  • Guido Hanauer,
  • Roeland Hanemaaijer

DOI
https://doi.org/10.1016/j.jcmgh.2017.10.001
Journal volume & issue
Vol. 5, no. 1
pp. 83 – 98.e10

Abstract

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The incidence of nonalcoholic steatohepatitis (NASH) is increasing. The pathophysiological mechanisms of NASH and the sequence of events leading to hepatic fibrosis are incompletely understood. The aim of this study was to gain insight into the dynamics of key molecular processes involved in NASH and to rank early markers for hepatic fibrosis. Methods: A time-course study in low-density lipoprotein–receptor knockout. Leiden mice on a high-fat diet was performed to identify the temporal dynamics of key processes contributing to NASH and fibrosis. An integrative systems biology approach was used to elucidate candidate markers linked to the active fibrosis process by combining transcriptomics, dynamic proteomics, and histopathology. The translational value of these findings were confirmed using human NASH data sets. Results: High-fat-diet feeding resulted in obesity, hyperlipidemia, insulin resistance, and NASH with fibrosis in a time-dependent manner. Temporal dynamics of key molecular processes involved in the development of NASH were identified, including lipid metabolism, inflammation, oxidative stress, and fibrosis. A data-integrative approach enabled identification of the active fibrotic process preceding histopathologic detection using a novel molecular fibrosis signature. Human studies were used to identify overlap of genes and processes and to perform a network biology-based prioritization to rank top candidate markers representing the early manifestation of fibrosis. Conclusions: An early predictive molecular signature was identified that marked the active profibrotic process before histopathologic fibrosis becomes manifest. Early detection of the onset of NASH and fibrosis enables identification of novel blood-based biomarkers to stratify patients at risk, development of new therapeutics, and help shorten (pre)clinical experimental time frames.

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