Atorvastatin provides a new lipidome improving early regeneration after partial hepatectomy in osteopontin deficient mice

Maitane Nuñez-Garcia,Virginia Gutiérrez-De Juan,Diego Saenz De Urturi,Beatriz Gomez-Santos,María Luz Martinez-Chantar,Xabier Buque,Olatz Fresnedo,Daniela Mestre,Francisco Gonzalez-Romero,Patricia Aspichueta,Wing-Kin Syn

doi:10.1038/s41598-018-32919-9

Abstract

Osteopontin (OPN), a multifunctional cytokine that controls liver glycerolipid metabolism, is involved in activation and proliferation of several liver cell types during regeneration, a condition of high metabolic demands. Here we investigated the role of OPN in modulating the liver lipidome during regeneration after partial-hepatectomy (PH) and the impact that atorvastatin treatment has over regeneration in OPN knockout (KO) mice. The results showed that OPN deficiency leads to remodeling of phosphatidylcholine and triacylglycerol (TG) species primarily during the first 24 h after PH, with minimal effects on regeneration. Changes in the quiescent liver lipidome in OPN-KO mice included TG enrichment with linoleic acid and were associated with higher lysosome TG-hydrolase activity that maintained 24 h after PH but increased in WT mice. OPN-KO mice showed increased beta-oxidation 24 h after PH with less body weight loss. In OPN-KO mice, atorvastatin treatment induced changes in the lipidome 24 h after PH and improved liver regeneration while no effect was observed 48 h post-PH. These results suggest that increased dietary-lipid uptake in OPN-KO mice provides the metabolic precursors required for regeneration 24 h and 48 h after PH. However, atorvastatin treatment offers a new metabolic program that improves early regeneration when OPN is deficient.

Highlights

The liver has the capacity for regeneration after cellular damage or surgery resection
We recently reported that OPN regulates PC and cholesterol metabolism cross-talk in the quiescent mouse liver and that OPN deficient mice exhibit decreased de novo fatty acids (FA) and TG synthesis in hepatocytes while liver TG content maintains unaltered[17]
OPN is a multifunctional cytokine involved in different liver disorders related with activation of a regenerative response, such as obesity related steatosis[25], non-alcoholic steatohepatitis[15], fibrosis[15], or hepatocellular carcinoma[26]

Summary

Introduction

The liver has the capacity for regeneration after cellular damage or surgery resection. Osteopontin (OPN) is a multifunctional cytokine that is expressed in various tissues[12,13] It plays an important role in obesity[12,14] and in fibrogenesis during non-alcoholic steatohepatitis (NASH) progression[15]. We investigated the roles of OPN in modulating liver TG and PC concentrations during liver regeneration after PH and the effects of atorvastatin on the regenerative liver lipidome in OPN deficient mice. Despite changes in PC concentration and PC and TG composition with OPN deficiency, remodeling of the liver lipid metabolism provides the metabolic precursors necessary for liver regeneration after PH. Treatment with atorvastatin ushered a new metabolic program that increased liver PC concentrations in OPN-KO mice 24 h after PH and promoted liver regeneration in these mice

Methods

Results

Conclusion