E-Selectin-Dependent Inflammation and Lipolysis in Adipose Tissue Exacerbate Steatosis-to-NASH Progression via S100A8/9

BACKGROUND & AIMS: Nonalcoholic steatohepatitis (NASH) is a leading cause of chronic liver disease, characterized by steatosis and hallmark liver neutrophil infiltration. NASH also is associated with adipose tissue inflammation, but the role of adipose tissue inflammation in NASH pathogenesis re...

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Autores principales: Rodrigues, Robim M., He, Yong, Hwang, Seonghwan, Bertola, Adeline, Mackowiak, Bryan, Ahmed, Yeni Ait, Seo, Wonhyo, Ma, Jing, Wang, Xiaolin, Park, Seol Hee, Guan, Yukun, Fu, Yaojie, Vanhaecke, Tamara, Feng, Dechun, Gao, Bin
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Elsevier 2021
Materias:
Original Research
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8593619/
https://www.ncbi.nlm.nih.gov/pubmed/34390865
http://dx.doi.org/10.1016/j.jcmgh.2021.08.002
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author Rodrigues, Robim M.
He, Yong
Hwang, Seonghwan
Bertola, Adeline
Mackowiak, Bryan
Ahmed, Yeni Ait
Seo, Wonhyo
Ma, Jing
Wang, Xiaolin
Park, Seol Hee
Guan, Yukun
Fu, Yaojie
Vanhaecke, Tamara
Feng, Dechun
Gao, Bin
author_facet Rodrigues, Robim M.
He, Yong
Hwang, Seonghwan
Bertola, Adeline
Mackowiak, Bryan
Ahmed, Yeni Ait
Seo, Wonhyo
Ma, Jing
Wang, Xiaolin
Park, Seol Hee
Guan, Yukun
Fu, Yaojie
Vanhaecke, Tamara
Feng, Dechun
Gao, Bin
author_sort Rodrigues, Robim M.
collection PubMed
description BACKGROUND & AIMS: Nonalcoholic steatohepatitis (NASH) is a leading cause of chronic liver disease, characterized by steatosis and hallmark liver neutrophil infiltration. NASH also is associated with adipose tissue inflammation, but the role of adipose tissue inflammation in NASH pathogenesis remains obscure. The aim of this study was to investigate the interplay between neutrophil recruitment in adipose tissue and the progression of NASH. METHODS: A mouse model of NASH was obtained by high-fat diet (HFD) feeding plus adenovirus-Cxcl1 overexpression (HFD(+AdCxcl1)). Genetic deletion of E-selectin (Sele) and treatment with an S100A9 inhibitor (Paquinimod) were investigated using this model. RESULTS: By analyzing transcriptomic data sets of adipose tissue from NASH patients, we found that E-selectin, a key adhesion molecule for neutrophils, is the highest up-regulated gene among neutrophil recruitment-related factors in adipose tissue of NASH patients compared with those in patients with simple steatosis. A marked up-regulation of Sele in adipose tissue also was observed in HFD(+AdCxcl1) mice. The HFD(+AdCxcl1)-induced NASH phenotype was ameliorated in Sele knockout mice and was accompanied by reduced lipolysis and inflammation in adipose tissue, which resulted in decreased serum free fatty acids and proinflammatory adipokines. S100A8/A9, a major proinflammatory protein secreted by neutrophils, was highly increased in adipose tissue of HFD(+AdCxcl1) mice. This increase was blunted in the Sele knockout mice. Therapeutically, treatment with the S100A9 inhibitor Paquinimod reduced lipolysis, inflammation, and adipokine production, ameliorating the NASH phenotype in mice. CONCLUSIONS: E-selectin plays an important role in inducing neutrophil recruitment in adipose tissue, which subsequently promotes inflammation and lipolysis via the production of S100A8/A9, thereby exacerbating the steatosis-to-NASH progression. Targeting adipose tissue inflammation therefore may represent a potential novel therapy for treatment of NASH.
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spelling pubmed-85936192021-11-22 E-Selectin-Dependent Inflammation and Lipolysis in Adipose Tissue Exacerbate Steatosis-to-NASH Progression via S100A8/9 Rodrigues, Robim M. He, Yong Hwang, Seonghwan Bertola, Adeline Mackowiak, Bryan Ahmed, Yeni Ait Seo, Wonhyo Ma, Jing Wang, Xiaolin Park, Seol Hee Guan, Yukun Fu, Yaojie Vanhaecke, Tamara Feng, Dechun Gao, Bin Cell Mol Gastroenterol Hepatol Original Research BACKGROUND & AIMS: Nonalcoholic steatohepatitis (NASH) is a leading cause of chronic liver disease, characterized by steatosis and hallmark liver neutrophil infiltration. NASH also is associated with adipose tissue inflammation, but the role of adipose tissue inflammation in NASH pathogenesis remains obscure. The aim of this study was to investigate the interplay between neutrophil recruitment in adipose tissue and the progression of NASH. METHODS: A mouse model of NASH was obtained by high-fat diet (HFD) feeding plus adenovirus-Cxcl1 overexpression (HFD(+AdCxcl1)). Genetic deletion of E-selectin (Sele) and treatment with an S100A9 inhibitor (Paquinimod) were investigated using this model. RESULTS: By analyzing transcriptomic data sets of adipose tissue from NASH patients, we found that E-selectin, a key adhesion molecule for neutrophils, is the highest up-regulated gene among neutrophil recruitment-related factors in adipose tissue of NASH patients compared with those in patients with simple steatosis. A marked up-regulation of Sele in adipose tissue also was observed in HFD(+AdCxcl1) mice. The HFD(+AdCxcl1)-induced NASH phenotype was ameliorated in Sele knockout mice and was accompanied by reduced lipolysis and inflammation in adipose tissue, which resulted in decreased serum free fatty acids and proinflammatory adipokines. S100A8/A9, a major proinflammatory protein secreted by neutrophils, was highly increased in adipose tissue of HFD(+AdCxcl1) mice. This increase was blunted in the Sele knockout mice. Therapeutically, treatment with the S100A9 inhibitor Paquinimod reduced lipolysis, inflammation, and adipokine production, ameliorating the NASH phenotype in mice. CONCLUSIONS: E-selectin plays an important role in inducing neutrophil recruitment in adipose tissue, which subsequently promotes inflammation and lipolysis via the production of S100A8/A9, thereby exacerbating the steatosis-to-NASH progression. Targeting adipose tissue inflammation therefore may represent a potential novel therapy for treatment of NASH. Elsevier 2021-08-11 /pmc/articles/PMC8593619/ /pubmed/34390865 http://dx.doi.org/10.1016/j.jcmgh.2021.08.002 Text en https://creativecommons.org/licenses/by-nc-nd/4.0/This is an open access article under the CC BY-NC-ND license (http://creativecommons.org/licenses/by-nc-nd/4.0/).
spellingShingle Original Research
Rodrigues, Robim M.
He, Yong
Hwang, Seonghwan
Bertola, Adeline
Mackowiak, Bryan
Ahmed, Yeni Ait
Seo, Wonhyo
Ma, Jing
Wang, Xiaolin
Park, Seol Hee
Guan, Yukun
Fu, Yaojie
Vanhaecke, Tamara
Feng, Dechun
Gao, Bin
E-Selectin-Dependent Inflammation and Lipolysis in Adipose Tissue Exacerbate Steatosis-to-NASH Progression via S100A8/9
title E-Selectin-Dependent Inflammation and Lipolysis in Adipose Tissue Exacerbate Steatosis-to-NASH Progression via S100A8/9
title_full E-Selectin-Dependent Inflammation and Lipolysis in Adipose Tissue Exacerbate Steatosis-to-NASH Progression via S100A8/9
title_fullStr E-Selectin-Dependent Inflammation and Lipolysis in Adipose Tissue Exacerbate Steatosis-to-NASH Progression via S100A8/9
title_full_unstemmed E-Selectin-Dependent Inflammation and Lipolysis in Adipose Tissue Exacerbate Steatosis-to-NASH Progression via S100A8/9
title_short E-Selectin-Dependent Inflammation and Lipolysis in Adipose Tissue Exacerbate Steatosis-to-NASH Progression via S100A8/9
title_sort e-selectin-dependent inflammation and lipolysis in adipose tissue exacerbate steatosis-to-nash progression via s100a8/9
topic Original Research
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8593619/
https://www.ncbi.nlm.nih.gov/pubmed/34390865
http://dx.doi.org/10.1016/j.jcmgh.2021.08.002
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