Characterization of sexual dimorphism in ANGPTL4 levels and function
ANGPTL4 is an attractive pharmacological target for lowering plasma triglycerides and cardiovascular risk. Since most preclinical studies on ANGPTL4 were performed in male mice, little is known about sexual dimorphism in ANGPTL4 regulation and function. Here, we aimed to study potential sexual dimorphism in ANGPTL4 mRNA and protein levels and ANGPTL4 function. Additionally, we performed exploratory studies on the function of ANGPTL4 in the liver during fasting using Angptl4-transgenic and Angptl4¡/¡ mice. Compared to female mice, male mice showed higher hepatic and adipose ANGPTL4 mRNA and protein levels, as well as a more pronounced effect of genetic ANGPTL4 modulation on plasma lipids. By contrast, very limited sexual dimorphism in ANGPTL4 levels was observed in human liver and adipose tissue. In human and mouse adipose tissue, ANGPTL8 mRNA and/or protein levels were significantly higher in females than males. Adipose LPL protein levels were higher in female than male Angptl4¡/¡ mice, which was abolished by ANGPTL4 (over) expression. At the human genetic level, the ANGPTL4 E40K loss-of-function variant was associated with similar plasma triglyceride reductions in women and men. Finally, ANGPTL4 ablation in fasted mice was associated with changes in hepatic gene expression consistent with PPARα activation. In conclusion, the levels of ANGPTL4 and the magnitude of the effect of ANGPTL4 on plasma lipids exhibit sexual dimorphism. Nonetheless, inactivation of ANGPTL4 should confer a similar metabolic benefit in women and men. Expression levels of ANGPTL8 in human and mouse adipose tissue are highly sexually dimorphic, showing higher levels in females than males.
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| Format: | Article/Letter to editor biblioteca |
| Language: | English |
| Subjects: | ANGPTL4, ANGPTL8, adipose tissue, lipase/lipoprotein, liver, sexual dimorphism, triglycerides, |
| Online Access: | https://research.wur.nl/en/publications/characterization-of-sexual-dimorphism-in-angptl4-levels-and-funct |
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dig-wur-nl-wurpubs-6298952025-01-14 Deng, Mingjuan Kersten, Sander Article/Letter to editor Journal of Lipid Research 65 (2024) 4 ISSN: 0022-2275 Characterization of sexual dimorphism in ANGPTL4 levels and function 2024 ANGPTL4 is an attractive pharmacological target for lowering plasma triglycerides and cardiovascular risk. Since most preclinical studies on ANGPTL4 were performed in male mice, little is known about sexual dimorphism in ANGPTL4 regulation and function. Here, we aimed to study potential sexual dimorphism in ANGPTL4 mRNA and protein levels and ANGPTL4 function. Additionally, we performed exploratory studies on the function of ANGPTL4 in the liver during fasting using Angptl4-transgenic and Angptl4¡/¡ mice. Compared to female mice, male mice showed higher hepatic and adipose ANGPTL4 mRNA and protein levels, as well as a more pronounced effect of genetic ANGPTL4 modulation on plasma lipids. By contrast, very limited sexual dimorphism in ANGPTL4 levels was observed in human liver and adipose tissue. In human and mouse adipose tissue, ANGPTL8 mRNA and/or protein levels were significantly higher in females than males. Adipose LPL protein levels were higher in female than male Angptl4¡/¡ mice, which was abolished by ANGPTL4 (over) expression. At the human genetic level, the ANGPTL4 E40K loss-of-function variant was associated with similar plasma triglyceride reductions in women and men. Finally, ANGPTL4 ablation in fasted mice was associated with changes in hepatic gene expression consistent with PPARα activation. In conclusion, the levels of ANGPTL4 and the magnitude of the effect of ANGPTL4 on plasma lipids exhibit sexual dimorphism. Nonetheless, inactivation of ANGPTL4 should confer a similar metabolic benefit in women and men. Expression levels of ANGPTL8 in human and mouse adipose tissue are highly sexually dimorphic, showing higher levels in females than males. en application/pdf https://research.wur.nl/en/publications/characterization-of-sexual-dimorphism-in-angptl4-levels-and-funct 10.1016/j.jlr.2024.100526 https://edepot.wur.nl/657813 ANGPTL4 ANGPTL8 adipose tissue lipase/lipoprotein liver sexual dimorphism triglycerides https://creativecommons.org/licenses/by/4.0/ https://creativecommons.org/licenses/by/4.0/ Wageningen University & Research |
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ANGPTL4 ANGPTL8 adipose tissue lipase/lipoprotein liver sexual dimorphism triglycerides ANGPTL4 ANGPTL8 adipose tissue lipase/lipoprotein liver sexual dimorphism triglycerides |
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ANGPTL4 ANGPTL8 adipose tissue lipase/lipoprotein liver sexual dimorphism triglycerides ANGPTL4 ANGPTL8 adipose tissue lipase/lipoprotein liver sexual dimorphism triglycerides Deng, Mingjuan Kersten, Sander Characterization of sexual dimorphism in ANGPTL4 levels and function |
| description |
ANGPTL4 is an attractive pharmacological target for lowering plasma triglycerides and cardiovascular risk. Since most preclinical studies on ANGPTL4 were performed in male mice, little is known about sexual dimorphism in ANGPTL4 regulation and function. Here, we aimed to study potential sexual dimorphism in ANGPTL4 mRNA and protein levels and ANGPTL4 function. Additionally, we performed exploratory studies on the function of ANGPTL4 in the liver during fasting using Angptl4-transgenic and Angptl4¡/¡ mice. Compared to female mice, male mice showed higher hepatic and adipose ANGPTL4 mRNA and protein levels, as well as a more pronounced effect of genetic ANGPTL4 modulation on plasma lipids. By contrast, very limited sexual dimorphism in ANGPTL4 levels was observed in human liver and adipose tissue. In human and mouse adipose tissue, ANGPTL8 mRNA and/or protein levels were significantly higher in females than males. Adipose LPL protein levels were higher in female than male Angptl4¡/¡ mice, which was abolished by ANGPTL4 (over) expression. At the human genetic level, the ANGPTL4 E40K loss-of-function variant was associated with similar plasma triglyceride reductions in women and men. Finally, ANGPTL4 ablation in fasted mice was associated with changes in hepatic gene expression consistent with PPARα activation. In conclusion, the levels of ANGPTL4 and the magnitude of the effect of ANGPTL4 on plasma lipids exhibit sexual dimorphism. Nonetheless, inactivation of ANGPTL4 should confer a similar metabolic benefit in women and men. Expression levels of ANGPTL8 in human and mouse adipose tissue are highly sexually dimorphic, showing higher levels in females than males. |
| format |
Article/Letter to editor |
| topic_facet |
ANGPTL4 ANGPTL8 adipose tissue lipase/lipoprotein liver sexual dimorphism triglycerides |
| author |
Deng, Mingjuan Kersten, Sander |
| author_facet |
Deng, Mingjuan Kersten, Sander |
| author_sort |
Deng, Mingjuan |
| title |
Characterization of sexual dimorphism in ANGPTL4 levels and function |
| title_short |
Characterization of sexual dimorphism in ANGPTL4 levels and function |
| title_full |
Characterization of sexual dimorphism in ANGPTL4 levels and function |
| title_fullStr |
Characterization of sexual dimorphism in ANGPTL4 levels and function |
| title_full_unstemmed |
Characterization of sexual dimorphism in ANGPTL4 levels and function |
| title_sort |
characterization of sexual dimorphism in angptl4 levels and function |
| url |
https://research.wur.nl/en/publications/characterization-of-sexual-dimorphism-in-angptl4-levels-and-funct |
| work_keys_str_mv |
AT dengmingjuan characterizationofsexualdimorphisminangptl4levelsandfunction AT kerstensander characterizationofsexualdimorphisminangptl4levelsandfunction |
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1822263075370172416 |