Amelioration of non-alcoholic fatty liver disease by targeting adhesion G protein-coupled receptor F1 (Adgrf1)

BACKGROUND: Recent research has shown that the adhesion G protein-coupled receptor F1 (Adgrf1; also known as GPR110; PGR19; KPG_012; hGPCR36) is an oncogene. The evidence is mainly based on high expression of Adgrf1 in numerous cancer types, and knockdown Adgrf1 can reduce the cell migration, invasi...

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Autores principales: Wu, Mengyao, Lo, Tak-Ho, Li, Liping, Sun, Jia, Deng, Chujun, Chan, Ka-Ying, Li, Xiang, Yeh, Steve Ting-Yuan, Lee, Jimmy Tsz Hang, Lui, Pauline Po Yee, Xu, Aimin, Wong, Chi-Ming
Formato: Online Artículo Texto
Lenguaje:English
Publicado: eLife Sciences Publications, Ltd 2023
Materias:
Cell Biology
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10427146/
https://www.ncbi.nlm.nih.gov/pubmed/37580962
http://dx.doi.org/10.7554/eLife.85131
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author Wu, Mengyao
Lo, Tak-Ho
Li, Liping
Sun, Jia
Deng, Chujun
Chan, Ka-Ying
Li, Xiang
Yeh, Steve Ting-Yuan
Lee, Jimmy Tsz Hang
Lui, Pauline Po Yee
Xu, Aimin
Wong, Chi-Ming
author_facet Wu, Mengyao
Lo, Tak-Ho
Li, Liping
Sun, Jia
Deng, Chujun
Chan, Ka-Ying
Li, Xiang
Yeh, Steve Ting-Yuan
Lee, Jimmy Tsz Hang
Lui, Pauline Po Yee
Xu, Aimin
Wong, Chi-Ming
author_sort Wu, Mengyao
collection PubMed
description BACKGROUND: Recent research has shown that the adhesion G protein-coupled receptor F1 (Adgrf1; also known as GPR110; PGR19; KPG_012; hGPCR36) is an oncogene. The evidence is mainly based on high expression of Adgrf1 in numerous cancer types, and knockdown Adgrf1 can reduce the cell migration, invasion, and proliferation. Adgrf1 is, however, mostly expressed in the liver of healthy individuals. The function of Adgrf1 in liver has not been revealed. Interestingly, expression level of hepatic Adgrf1 is dramatically decreased in obese subjects. Here, the research examined whether Adgrf1 has a role in liver metabolism. METHODS: We used recombinant adeno-associated virus-mediated gene delivery system, and antisense oligonucleotide was used to manipulate the hepatic Adgrf1 expression level in diet-induced obese mice to investigate the role of Adgrf1 in hepatic steatosis. The clinical relevance was examined using transcriptome profiling and archived biopsy specimens of liver tissues from non-alcoholic fatty liver disease (NAFLD) patients with different degree of fatty liver. RESULTS: The expression of Adgrf1 in the liver was directly correlated to fat content in the livers of both obese mice and NAFLD patients. Stearoyl-coA desaturase 1 (Scd1), a crucial enzyme in hepatic de novo lipogenesis, was identified as a downstream target of Adgrf1 by RNA-sequencing analysis. Treatment with the liver-specific Scd1 inhibitor MK8245 and specific shRNAs against Scd1 in primary hepatocytes improved the hepatic steatosis of Adgrf1-overexpressing mice and lipid profile of hepatocytes, respectively. CONCLUSIONS: These results indicate Adgrf1 regulates hepatic lipid metabolism through controlling the expression of Scd1. Downregulation of Adgrf1 expression can potentially serve as a protective mechanism to stop the overaccumulation of fat in the liver in obese subjects. Overall, the above findings not only reveal a new mechanism regulating the progression of NAFLD, but also proposed a novel therapeutic approach to combat NAFLD by targeting Adgrf1. FUNDING: This work was supported by the National Natural Science Foundation of China (81870586), Area of Excellence (AoE/M-707/18), and General Research Fund (15101520) to CMW, and the National Natural Science Foundation of China (82270941, 81974117) to SJ.
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spelling pubmed-104271462023-08-16 Amelioration of non-alcoholic fatty liver disease by targeting adhesion G protein-coupled receptor F1 (Adgrf1) Wu, Mengyao Lo, Tak-Ho Li, Liping Sun, Jia Deng, Chujun Chan, Ka-Ying Li, Xiang Yeh, Steve Ting-Yuan Lee, Jimmy Tsz Hang Lui, Pauline Po Yee Xu, Aimin Wong, Chi-Ming eLife Cell Biology BACKGROUND: Recent research has shown that the adhesion G protein-coupled receptor F1 (Adgrf1; also known as GPR110; PGR19; KPG_012; hGPCR36) is an oncogene. The evidence is mainly based on high expression of Adgrf1 in numerous cancer types, and knockdown Adgrf1 can reduce the cell migration, invasion, and proliferation. Adgrf1 is, however, mostly expressed in the liver of healthy individuals. The function of Adgrf1 in liver has not been revealed. Interestingly, expression level of hepatic Adgrf1 is dramatically decreased in obese subjects. Here, the research examined whether Adgrf1 has a role in liver metabolism. METHODS: We used recombinant adeno-associated virus-mediated gene delivery system, and antisense oligonucleotide was used to manipulate the hepatic Adgrf1 expression level in diet-induced obese mice to investigate the role of Adgrf1 in hepatic steatosis. The clinical relevance was examined using transcriptome profiling and archived biopsy specimens of liver tissues from non-alcoholic fatty liver disease (NAFLD) patients with different degree of fatty liver. RESULTS: The expression of Adgrf1 in the liver was directly correlated to fat content in the livers of both obese mice and NAFLD patients. Stearoyl-coA desaturase 1 (Scd1), a crucial enzyme in hepatic de novo lipogenesis, was identified as a downstream target of Adgrf1 by RNA-sequencing analysis. Treatment with the liver-specific Scd1 inhibitor MK8245 and specific shRNAs against Scd1 in primary hepatocytes improved the hepatic steatosis of Adgrf1-overexpressing mice and lipid profile of hepatocytes, respectively. CONCLUSIONS: These results indicate Adgrf1 regulates hepatic lipid metabolism through controlling the expression of Scd1. Downregulation of Adgrf1 expression can potentially serve as a protective mechanism to stop the overaccumulation of fat in the liver in obese subjects. Overall, the above findings not only reveal a new mechanism regulating the progression of NAFLD, but also proposed a novel therapeutic approach to combat NAFLD by targeting Adgrf1. FUNDING: This work was supported by the National Natural Science Foundation of China (81870586), Area of Excellence (AoE/M-707/18), and General Research Fund (15101520) to CMW, and the National Natural Science Foundation of China (82270941, 81974117) to SJ. eLife Sciences Publications, Ltd 2023-08-15 /pmc/articles/PMC10427146/ /pubmed/37580962 http://dx.doi.org/10.7554/eLife.85131 Text en © 2023, Wu 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
Wu, Mengyao
Lo, Tak-Ho
Li, Liping
Sun, Jia
Deng, Chujun
Chan, Ka-Ying
Li, Xiang
Yeh, Steve Ting-Yuan
Lee, Jimmy Tsz Hang
Lui, Pauline Po Yee
Xu, Aimin
Wong, Chi-Ming
Amelioration of non-alcoholic fatty liver disease by targeting adhesion G protein-coupled receptor F1 (Adgrf1)
title Amelioration of non-alcoholic fatty liver disease by targeting adhesion G protein-coupled receptor F1 (Adgrf1)
title_full Amelioration of non-alcoholic fatty liver disease by targeting adhesion G protein-coupled receptor F1 (Adgrf1)
title_fullStr Amelioration of non-alcoholic fatty liver disease by targeting adhesion G protein-coupled receptor F1 (Adgrf1)
title_full_unstemmed Amelioration of non-alcoholic fatty liver disease by targeting adhesion G protein-coupled receptor F1 (Adgrf1)
title_short Amelioration of non-alcoholic fatty liver disease by targeting adhesion G protein-coupled receptor F1 (Adgrf1)
title_sort amelioration of non-alcoholic fatty liver disease by targeting adhesion g protein-coupled receptor f1 (adgrf1)
topic Cell Biology
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10427146/
https://www.ncbi.nlm.nih.gov/pubmed/37580962
http://dx.doi.org/10.7554/eLife.85131
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