[HTML][HTML] Cell fate analysis of zone 3 hepatocytes in liver injury and tumorigenesis
S Kurosaki, H Nakagawa, Y Hayata, S Kawamura… - JHEP Reports, 2021 - Elsevier
S Kurosaki, H Nakagawa, Y Hayata, S Kawamura, Y Matsushita, T Yamada, K Uchino…
JHEP Reports, 2021•ElsevierBackground & Aims Liver lobules are typically subdivided into 3 metabolic zones: zones 1,
2, and 3. However, the contribution of zonal differences in hepatocytes to liver regeneration,
as well as to carcinogenic susceptibility, remains unclear. Methods We developed a new
method for sustained genetic labelling of zone 3 hepatocytes and performed fate tracing to
monitor these cells in multiple mouse liver tumour models. Results We first examined
changes in the zonal distribution of the Wnt target gene Axin2 over time using Axin2-Cre …
2, and 3. However, the contribution of zonal differences in hepatocytes to liver regeneration,
as well as to carcinogenic susceptibility, remains unclear. Methods We developed a new
method for sustained genetic labelling of zone 3 hepatocytes and performed fate tracing to
monitor these cells in multiple mouse liver tumour models. Results We first examined
changes in the zonal distribution of the Wnt target gene Axin2 over time using Axin2-Cre …
Background & Aims
Liver lobules are typically subdivided into 3 metabolic zones: zones 1, 2, and 3. However, the contribution of zonal differences in hepatocytes to liver regeneration, as well as to carcinogenic susceptibility, remains unclear.
Methods
We developed a new method for sustained genetic labelling of zone 3 hepatocytes and performed fate tracing to monitor these cells in multiple mouse liver tumour models.
Results
We first examined changes in the zonal distribution of the Wnt target gene Axin2 over time using Axin2-CreERT2;Rosa26-Lox-Stop-Lox-tdTomato mice (Axin2;tdTomato). We found that following tamoxifen administration at 3 weeks of age, approximately one-third of total hepatocytes that correspond to zone 3 were labelled in Axin2;tdTomato mice; the tdTomato+ cell distribution closely matched that of the zone 3 marker CYP2E1. Cell fate analysis revealed that zone 3 hepatocytes maintained their own lineage but rarely proliferated beyond their liver zonation during homoeostasis; this indicated that our protocol enabled persistent genetic labelling of zone 3 hepatocytes. Using this system, we found that zone 3 hepatocytes generally had high neoplastic potential, which was promoted by constitutive activation of Wnt/β-catenin signalling in the pericentral area. However, the frequency of zone 3 hepatocyte-derived tumours varied depending on the regeneration pattern of the liver parenchyma in response to liver injury. Notably, Axin2-expressing hepatocytes undergoing chronic liver injury significantly contributed to liver regeneration and possessed high neoplastic potential. Additionally, we revealed that the metabolic phenotypes of liver tumours were acquired during tumorigenesis, irrespective of their spatial origin.
Conclusions
Hepatocytes receiving Wnt/β-catenin signalling from their microenvironment have high neoplastic potential, and Wnt/β-catenin signalling is a potential drug target for the prevention of hepatocellular carcinoma.
Lay summary
Lineage tracing revealed that zone 3 hepatocytes residing in the pericentral niche have high neoplastic potential. Under chronic liver injury, hepatocytes receiving Wnt/β-catenin signalling broadly exist across all hepatic zones and significantly contribute to liver tumorigenesis as well as liver regeneration. Wnt/β-catenin signalling is a potential drug target for the prevention of hepatocellular carcinoma.
Elsevier
