ACOT1 deficiency attenuates high-fat diet–induced fat mass gain by increasing energy expenditure
Timothy D. Heden, … , Chen Chen, Douglas G. Mashek
Timothy D. Heden, … , Chen Chen, Douglas G. Mashek
Published August 10, 2023
Citation Information: JCI Insight. 2023;8(18):e160987. https://doi.org/10.1172/jci.insight.160987.
View: Text | PDF
Research Article Metabolism

ACOT1 deficiency attenuates high-fat diet–induced fat mass gain by increasing energy expenditure

Abstract

Acyl-CoA thioesterase 1 (ACOT1) catalyzes the hydrolysis of long-chain acyl-CoAs to free fatty acids and CoA and is typically upregulated in obesity. Whether targeting ACOT1 in the setting of high-fat diet–induced (HFD-induced) obesity would be metabolically beneficial is not known. Here we report that male and female ACOT1KO mice are partially protected from HFD-induced obesity, an effect associated with increased energy expenditure without alterations in physical activity or food intake. In males, ACOT1 deficiency increased mitochondrial uncoupling protein-2 (UCP2) protein abundance while reducing 4-hydroxynonenal, a marker of oxidative stress, in white adipose tissue and liver of HFD-fed mice. Moreover, concurrent knockdown (KD) of UCP2 with ACOT1 in hepatocytes prevented increases in oxygen consumption observed with ACOT1 KD during high lipid loading, suggesting that UCP2-induced uncoupling may increase energy expenditure to attenuate weight gain. Together, these data indicate that targeting ACOT1 may be effective for obesity prevention during caloric excess by increasing energy expenditure.

Authors

Timothy D. Heden, Mallory P. Franklin, Christina Dailey, Mara T. Mashek, Chen Chen, Douglas G. Mashek

×

Figure 1

ACOT1KO modestly attenuates HFD-induced fat weight gain in male mice.

Options: View larger image (or click on image) Download as PowerPoint
ACOT1KO modestly attenuates HFD-induced fat weight gain in male mice. (A...
(A) VelociGene KOMP null allele design. (B) Southern blot image showing WT, heterozygous (Het), and homozygous (KO) bands for genotyping. (C) ACOT1 mRNA abundance in liver, iWAT, gWAT, and BAT in 20-week-old control male mice fed the LFD for 12 weeks, ACOT1KO mice fed the LFD for 12 weeks, control mice fed the HFD for 12 weeks, and ACOT1KO mice fed the HFD for 12 weeks (n = 2–11 per group). (D) Western blot images of ACOT1 in liver and BAT tissues (n = 2 per group). (E) Liver thioesterase activity (n = 4–5 per group). (F) BW time course (n = 16–24 per group). (G) BW gain during each diet (n = 16–23 per group). (H) Echo MRI body composition data (n = 9–10 per group). All data are presented as mean ± SEM. An ANOVA (G used 1 way; C, D, F, and H used a 2 way) or 2-tailed t test (E) was used for statistical tests. aP ≤ 0.01 control LFD versus control HFD, bP = 0.02 ACOT1KO LFD versus ACOT1KO HFD, and cP ≤ 0.01 control HFD versus ACOT1KO HFD.