PLoS ONE (Jan 2015)

Reciprocal interaction of Wnt and RXR-α pathways in hepatocyte development and hepatocellular carcinoma.

  • Jinyu Li,
  • Maia Chanrion,
  • Eric Sawey,
  • Tim Wang,
  • Edward Chow,
  • Aaron Tward,
  • Yi Su,
  • Wen Xue,
  • Robert Lucito,
  • Lars Zender,
  • Scott W Lowe,
  • J Michael Bishop,
  • Scott Powers

DOI
https://doi.org/10.1371/journal.pone.0118480
Journal volume & issue
Vol. 10, no. 3
p. e0118480

Abstract

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Genomic analysis of human hepatocellular carcinoma (HCC) is potentially confounded by the differentiation state of the hepatic cell-of-origin. Here we integrated genomic analysis of mouse HCC (with defined cell-of-origin) along with normal development. We found a major shift in expression of Wnt and RXR-α pathway genes (up and down, respectively) coincident with the transition from hepatoblasts to hepatocytes. A combined Wnt and RXR-α gene signature categorized HCCs into two subtypes (high Wnt, low RXR-α and low Wnt, high RXR-α), which matched cell-of-origin in mouse models and the differentiation state of human HCC. Suppression of RXR-α levels in hepatocytes increased Wnt signaling and enhanced tumorigenicity, whereas ligand activation of RXR-α achieved the opposite. These results corroborate that there are two main HCC subtypes that correspond to the degree of hepatocyte differentation and that RXR-α, in part via Wnt signaling, plays a key functional role in the hepatocyte-like subtype and potentially could serve as a selective therapeutic target.