Enhanced Liver Regeneration Following Changes Induced by Hepatocyte-specific Genetic Ablation of Integrin-linked Kinase

Overview

Journal Hepatology

Specialty Gastroenterology

Date 2009 Jul 4

PMID 19575460

Citations 75

Authors

Udayan Apte

Vasiliki Gkretsi

William C Bowen

Wendy M Mars

Jian-Hua Luo

Shashikiran Donthamsetty

Ann Orr

Satdarshan P S Monga

Chuanyue Wu

George K Michalopoulos

Affiliations

Soon will be listed here.

Abstract

Unlabelled: Following liver regeneration after partial hepatectomy, liver grows back precisely to its original mass and does not exceed it. The mechanism regulating this "hepatostat" is not clear and no exceptions have been found to date. Although pathways initiating liver regeneration have been well studied, mechanisms involved in the termination of liver regeneration are unclear. Here, we report that integrin-linked kinase (ILK) (involved in transmission of the extracellular matrix [ECM] signaling by way of integrin receptors) and/or hepatic adaptations that ensue following ILK hepatocyte-targeted removal are critical for proper termination of liver regeneration. Following partial hepatectomy (PHx), mice with a liver-specific ILK ablation (ILK-KO-Liver) demonstrate a termination defect resulting in 58% larger liver than their original pre-PHx mass. This increase in post-PHx liver mass is due to sustained cell proliferation driven in part by increased signaling through hepatocyte growth factor (HGF), and the beta-catenin pathway and Hippo kinase pathways.

Conclusion: The data indicate that ECM-mediated signaling by way of ILK is essential in proper termination of liver regeneration. This is the first evidence of a defect leading to impaired termination of regeneration and excessive accumulation of liver weight following partial hepatectomy.

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