Title

Raldh1 Promotes Adiposity During Adolescence Independently of Retinal Signaling

Authors

Di Yang, University of California, Berkeley
Charles Krois, Minnesota State Univeristy, Mankato
Priscilla Huang, University of California, Berkeley
Jinshan Wang, University of California, Berkeley
Jin Min, University of California, Berkeley
Hong Yoo, University of California, Berkeley
Yinghua Deng, University of California, Berkeley
Joseph Napoli, University of California, Berkeley
Michael Schubert, École normale supérieure de Lyon

Document Type

Article

Publication Date

2-11-2017

Abstract

All-trans-retinoic acid (RA) inhibits adipogenesis in established preadipocyte cell lines. Dosing pharmacological amounts of RA reduces weight gain in mice fed a high-fat diet, i.e. counteracts diet-induced obesity (DIO). The aldehyde dehydrogenase Raldh1 (Aldh1a1) functions as one of three enzymes that converts the retinol metabolite retinal into RA, and one of many proteins that contribute to RA homeostasis. Female Raldh1-ablated mice resist DIO. This phenotype contrasts with ablations of other enzymes and binding-proteins that maintain RA homeostasis, which gain adiposity. The phenotype observed prompted the conclusion that loss of Raldh1 causes an increase in adipose tissue retinal, and therefore, retinal functions independently of RA to prevent DIO. A second deduction proposed that low nM concentrations of RA stimulate adipogenesis, in contrast to higher concentrations. Using peer-reviewed LC/MS/MS assays developed and validated for quantifying tissue RA and retinal, we show that endogenous retinal and RA concentrations in adipose tissues from Raldh1-null mice do not correlate with the phenotype. Moreover, male Raldh1-null mice resist weight gain regardless of dietary fat content. Resistance to weight gain occurs during adolescence in both sexes. We show that RA concentrations as low as 1 nM, i.e. in the sub-physiological range, impair adipogenesis of embryonic fibroblasts from wild-type mice. Embryonic fibroblasts from Raldh1-null mice resist differentiating into adipocytes, but retain ability to generate RA. These fibroblasts remain sensitive to an RA receptor pan-agonist, and are not affected by an RA receptor pan-antagonist. Thus, the data do not support the hypothesis that retinal itself represses weight gain and adipogenesis independently of RA. Instead, the data indicate that Raldh1 functions as a retinal and atRA-independent promoter of adiposity during adolescence, and enhances adiposity through pre-adipocyte cell autonomous actions.

Department

Chemistry and Geology

Print ISSN

1932-6203

Publication Title

PLOS ONE

Recommended Citation

Yang D, Krois CR, Huang P, Wang J, Min J, Yoo HS, et al. (2017) Raldh1 promotes adiposity during adolescence independently of retinal signaling. PLoS ONE 12(11): e0187669. https://doi. org/10.1371/journal.pone.0187669

DOI

10.1371/journal.pone.0187669

Link to Publisher Version (DOI)

https://doi.org/10.1371/journal.pone.0187669

Publisher's Copyright and Source

Copyright © 2017 Yang et al.