Remodeling of whole-body lipid metabolism and a diabetic-like phenotype caused by loss of CDK1 and hepatocyte division

Cell cycle progression and lipid metabolism are well-coordinated processes required for proper cell proliferation. In liver diseases that arise from dysregulated lipid metabolism, hepatocyte proliferation is diminished. To study the outcome of CDK1 loss and blocked hepatocyte proliferation on lipid...

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Autores principales: Ow, Jin Rong, Caldez, Matias J, Zafer, Gözde, Foo, Juat Chin, Li, Hong Yu, Ghosh, Soumita, Wollmann, Heike, Cazenave-Gassiot, Amaury, Ong, Chee Bing, Wenk, Markus R, Han, Weiping, Choi, Hyungwon, Kaldis, Philipp
Formato: Online Artículo Texto
Lenguaje:English
Publicado: eLife Sciences Publications, Ltd 2020
Materias:
Cell Biology
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7771968/
https://www.ncbi.nlm.nih.gov/pubmed/33345777
http://dx.doi.org/10.7554/eLife.63835
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author Ow, Jin Rong
Caldez, Matias J
Zafer, Gözde
Foo, Juat Chin
Li, Hong Yu
Ghosh, Soumita
Wollmann, Heike
Cazenave-Gassiot, Amaury
Ong, Chee Bing
Wenk, Markus R
Han, Weiping
Choi, Hyungwon
Kaldis, Philipp
author_facet Ow, Jin Rong
Caldez, Matias J
Zafer, Gözde
Foo, Juat Chin
Li, Hong Yu
Ghosh, Soumita
Wollmann, Heike
Cazenave-Gassiot, Amaury
Ong, Chee Bing
Wenk, Markus R
Han, Weiping
Choi, Hyungwon
Kaldis, Philipp
author_sort Ow, Jin Rong
collection PubMed
description Cell cycle progression and lipid metabolism are well-coordinated processes required for proper cell proliferation. In liver diseases that arise from dysregulated lipid metabolism, hepatocyte proliferation is diminished. To study the outcome of CDK1 loss and blocked hepatocyte proliferation on lipid metabolism and the consequent impact on whole-body physiology, we performed lipidomics, metabolomics, and RNA-seq analyses on a mouse model. We observed reduced triacylglycerides in liver of young mice, caused by oxidative stress that activated FOXO1 to promote the expression of Pnpla2/ATGL. Additionally, we discovered that hepatocytes displayed malfunctioning β-oxidation, reflected by increased acylcarnitines (ACs) and reduced β-hydroxybutyrate. This led to elevated plasma free fatty acids (FFAs), which were transported to the adipose tissue for storage and triggered greater insulin secretion. Upon aging, chronic hyperinsulinemia resulted in insulin resistance and hepatic steatosis through activation of LXR. Here, we demonstrate that loss of hepatocyte proliferation is not only an outcome but also possibly a causative factor for liver pathology.
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spelling pubmed-77719682020-12-30 Remodeling of whole-body lipid metabolism and a diabetic-like phenotype caused by loss of CDK1 and hepatocyte division Ow, Jin Rong Caldez, Matias J Zafer, Gözde Foo, Juat Chin Li, Hong Yu Ghosh, Soumita Wollmann, Heike Cazenave-Gassiot, Amaury Ong, Chee Bing Wenk, Markus R Han, Weiping Choi, Hyungwon Kaldis, Philipp eLife Cell Biology Cell cycle progression and lipid metabolism are well-coordinated processes required for proper cell proliferation. In liver diseases that arise from dysregulated lipid metabolism, hepatocyte proliferation is diminished. To study the outcome of CDK1 loss and blocked hepatocyte proliferation on lipid metabolism and the consequent impact on whole-body physiology, we performed lipidomics, metabolomics, and RNA-seq analyses on a mouse model. We observed reduced triacylglycerides in liver of young mice, caused by oxidative stress that activated FOXO1 to promote the expression of Pnpla2/ATGL. Additionally, we discovered that hepatocytes displayed malfunctioning β-oxidation, reflected by increased acylcarnitines (ACs) and reduced β-hydroxybutyrate. This led to elevated plasma free fatty acids (FFAs), which were transported to the adipose tissue for storage and triggered greater insulin secretion. Upon aging, chronic hyperinsulinemia resulted in insulin resistance and hepatic steatosis through activation of LXR. Here, we demonstrate that loss of hepatocyte proliferation is not only an outcome but also possibly a causative factor for liver pathology. eLife Sciences Publications, Ltd 2020-12-21 /pmc/articles/PMC7771968/ /pubmed/33345777 http://dx.doi.org/10.7554/eLife.63835 Text en © 2020, Ow et al https://creativecommons.org/licenses/by/4.0/This article is distributed under the terms of the Creative Commons Attribution License (https://creativecommons.org/licenses/by/4.0/) , which permits unrestricted use and redistribution provided that the original author and source are credited.
spellingShingle Cell Biology
Ow, Jin Rong
Caldez, Matias J
Zafer, Gözde
Foo, Juat Chin
Li, Hong Yu
Ghosh, Soumita
Wollmann, Heike
Cazenave-Gassiot, Amaury
Ong, Chee Bing
Wenk, Markus R
Han, Weiping
Choi, Hyungwon
Kaldis, Philipp
Remodeling of whole-body lipid metabolism and a diabetic-like phenotype caused by loss of CDK1 and hepatocyte division
title Remodeling of whole-body lipid metabolism and a diabetic-like phenotype caused by loss of CDK1 and hepatocyte division
title_full Remodeling of whole-body lipid metabolism and a diabetic-like phenotype caused by loss of CDK1 and hepatocyte division
title_fullStr Remodeling of whole-body lipid metabolism and a diabetic-like phenotype caused by loss of CDK1 and hepatocyte division
title_full_unstemmed Remodeling of whole-body lipid metabolism and a diabetic-like phenotype caused by loss of CDK1 and hepatocyte division
title_short Remodeling of whole-body lipid metabolism and a diabetic-like phenotype caused by loss of CDK1 and hepatocyte division
title_sort remodeling of whole-body lipid metabolism and a diabetic-like phenotype caused by loss of cdk1 and hepatocyte division
topic Cell Biology
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7771968/
https://www.ncbi.nlm.nih.gov/pubmed/33345777
http://dx.doi.org/10.7554/eLife.63835
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