NUDT7 regulates total hepatic CoA levels and the composition of the intestinal bile acid pool in male mice fed a Western diet

Nudix hydrolase 7 (NUDT7) is an enzyme that hydrolyzes CoA species, is highly expressed in the liver, and resides in the peroxisomes. Peroxisomes are organelles where the preferential oxidation of dicarboxylic fatty acids occurs and where the hepatic synthesis of the primary bile acids cholic acid a...

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Published in:The Journal of biological chemistry 2023-01, Vol.299 (1), p.102745-102745, Article 102745
Main Authors: Vickers, Schuyler D., Shumar, Stephanie A., Saporito, Dominique C., Kunovac, Amina, Hathaway, Quincy A., Mintmier, Breeanna, King, Judy A., King, Rachel D., Rajendran, Vazhaikkurichi M., Infante, Aniello M., Hollander, John M., Leonardi, Roberta
Format: Article
Language:English
Subjects:
Acyl Coenzyme A - metabolism
Animals
bile acids
Bile Acids and Salts - metabolism
Chenodeoxycholic Acid
cholesterol
dicarboxylic fatty acids
Diet, Western
Fatty Acids - metabolism
Liver - metabolism
Male
Mice
Nudix Hydrolases
Oxidation-Reduction
peroxisomes
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Summary:Nudix hydrolase 7 (NUDT7) is an enzyme that hydrolyzes CoA species, is highly expressed in the liver, and resides in the peroxisomes. Peroxisomes are organelles where the preferential oxidation of dicarboxylic fatty acids occurs and where the hepatic synthesis of the primary bile acids cholic acid and chenodeoxycholic acid is completed. We previously showed that liver-specific overexpression of NUDT7 affects peroxisomal lipid metabolism but does not prevent the increase in total liver CoA levels that occurs during fasting. We generated Nudt7-/- mice to further characterize the role that peroxisomal (acyl-)CoA degradation plays in the modulation of the size and composition of the acyl-CoA pool and in the regulation of hepatic lipid metabolism. Here, we show that deletion of Nudt7 alters the composition of the hepatic acyl-CoA pool in mice fed a low-fat diet, but only in males fed a Western diet does the lack of NUDT7 activity increase total liver CoA levels. This effect is driven by the male-specific accumulation of medium-chain dicarboxylic acyl-CoAs, which are produced from the β-oxidation of dicarboxylic fatty acids. We also show that, under conditions of elevated synthesis of chenodeoxycholic acid derivatives, Nudt7 deletion promotes the production of tauromuricholic acid, decreasing the hydrophobicity index of the intestinal bile acid pool and increasing fecal cholesterol excretion in male mice. These findings reveal that NUDT7-mediated hydrolysis of acyl-CoA pathway intermediates in liver peroxisomes contributes to the regulation of dicarboxylic fatty acid metabolism and the composition of the bile acid pool.
ISSN:0021-9258
1083-351X
DOI:10.1016/j.jbc.2022.102745