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LDB1 Regulates Energy Homeostasis During Diet-Induced Obesity.

Citation
Loyd, C., et al. “Ldb1 Regulates Energy Homeostasis During Diet-Induced Obesity.”. Endocrinology, pp. 1289-1297.
Center University of Alabama at Birmingham
Author Christine Loyd, Yanping Liu, Teayoun Kim, Cassie Holleman, Jamie Galloway, Maigen Bethea, Benjamin N Ediger, Thomas A Swain, Yawen Tang, Doris A Stoffers, Glenn C Rowe, Martin Young, Chad Steele, Kirk M Habegger, Chad S Hunter
Abstract

The broadly expressed transcriptional coregulator LDB1 is essential for β-cell development and glucose homeostasis. However, it is unclear whether LDB1 has metabolic roles beyond the β-cell, especially under metabolic stress. Global Ldb1 deletion results in early embryonic lethality; thus, we used global heterozygous Ldb1+/- and inducible β-cell-specific Ldb1-deficient (Ldb1Δβ-cell) mice. We assessed glucose and insulin tolerance, body composition, feeding, and energy expenditure during high-fat diet exposure. Brown adipose tissue (BAT) biology was evaluated by thermogenic gene expression and LDB1 chromatin immunoprecipitation analysis. We found that partial loss of Ldb1 does not impair the maintenance of glucose homeostasis; rather, we observed improved insulin sensitivity in these mice. Partial loss of Ldb1 also uncovered defects in energy expenditure in lean and diet-induced obese (DIO) mice. This decreased energy expenditure during DIO was associated with significantly altered BAT gene expression, specifically Cidea, Elovl3, Cox7a1, and Dio2. Remarkably, the observed changes in energy balance during DIO were absent in Ldb1Δβ-cell mice, despite a similar reduction in plasma insulin, suggesting a role for LDB1 in BAT. Indeed, LDB1 is expressed in brown adipocytes and occupies a regulatory domain of Elovl3, a gene crucial to normal BAT function. We conclude that LDB1 regulates energy homeostasis, in part through transcriptional modulation of critical regulators in BAT function.

Year of Publication
2017
Journal
Endocrinology
Volume
158
Issue
5
Number of Pages
1289-1297
Date Published
12/2017
ISSN Number
1945-7170
DOI
10.1210/en.2016-1791
Alternate Journal
Endocrinology
PMID
28009534
PMCID
PMC5460834
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