Publication date: 20 February 2018
Source:Cell Reports, Volume 22, Issue 8
Author(s): Vanessa Maillet, Nadia Boussetta, Jocelyne Leclerc, Véronique Fauveau, Marc Foretz, Benoit Viollet, Jean-Pierre Couty, Séverine Celton-Morizur, Christine Perret, Chantal Desdouets
Liver kinase B1 (LKB1) is involved in several biological processes and is a key regulator of hepatic metabolism and polarity. Here, we demonstrate that the master kinase LKB1 plays a dual role in liver regeneration, independently of its major target, AMP-activated protein kinase (AMPK). We found that the loss of hepatic Lkb1 expression promoted hepatocyte proliferation acceleration independently of metabolic/energetic balance. LKB1 regulates G0/G1 progression, specifically by controlling epidermal growth factor receptor (EGFR) signaling. Furthermore, later in regeneration, LKB1 controls mitotic fidelity. The deletion of Lkb1 results in major alterations to mitotic spindle formation along the polarity axis. Thus, LKB1 deficiency alters ploidy profile at late stages of regeneration. Our findings highlight the dual role of LKB1 in liver regeneration, as a guardian of hepatocyte proliferation and genomic integrity.
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Teaser
Maillet et al. demonstrate that the master kinase LKB1 plays a dual role in liver regeneration, independently of its major target, AMPK. LKB1 acts as a guardian of hepatocyte proliferation by controlling G0/G1 transition through EGFR activation. These findings also show that LKB1 is a gatekeeper of mitotic fidelity and hepatocyte ploidy integrity.http://ift.tt/2GHrcgK
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