| Literature DB >> 31504388 |
Wei Wang1,2, Xiao Hao1,2, Lina Han1,2, Zhe Yan1,2, Wen-Jun Shen1,2, Dachuan Dong1,2, Kathrin Hasbargen1,2, Stefanie Bittner2, Yuan Cortez1,2, Andrew S Greenberg3, Salman Azhar1,2, Fredric B Kraemer1,2.
Abstract
ACSL4 is a member of the ACSL family that catalyzes the conversion of long-chain fatty acids to acyl-coenzyme As, which are essential for fatty-acid incorporation and utilization in diverse metabolic pathways, including cholesteryl ester synthesis. Steroidogenic tissues such as the adrenal gland are particularly enriched in cholesteryl esters of long-chain polyunsaturated fatty acids, which constitute an important pool supplying cholesterol for steroid synthesis. The current studies addressed whether ACSL4 is required for normal steroidogenesis. CYP11A1 promoter‒mediated Cre was used to generate steroid tissue‒specific ACSL4 knockout (KO) mice. Results demonstrated that ACSL4 plays an important role in adrenal cholesteryl ester formation, as well as in determining the fatty acyl composition of adrenal cholesteryl esters, with ACSL4 deficiency leading to reductions in cholesteryl ester storage and alterations in cholesteryl ester composition. Statistically significant reductions in corticosterone and testosterone production, but not progesterone production, were observed in vivo, and these deficits were accentuated in ex vivo and in vitro studies of isolated steroid tissues and cells from ACSL4-deficient mice. However, these effects on steroid production appear to be due to reductions in cholesteryl ester stores rather than disturbances in signaling pathways. We conclude that ACSL4 is dispensable for normal steroidogenesis. Published by Oxford University Press on behalf of the Endocrine Society 2019.Entities:
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Year: 2019 PMID: 31504388 PMCID: PMC6773434 DOI: 10.1210/en.2019-00464
Source DB: PubMed Journal: Endocrinology ISSN: 0013-7227 Impact factor: 4.736