LncRNA U90926 is dispensable for the development of obesity‐associated phenotypes in vivo

Author:

Sabikunnahar Bristy1,Caldwell Sydney1,Varnum Stella1,Hogan Tyler1,Lahue Karolyn G.1,Rathkolb Birgit234,Gerlini Raffaele2,Dragano Nathalia R. V.23,Aguilar‐Pimentel Antonio2,Irmler Martin2,Sanz‐Moreno Adrián2,da Silva‐Buttkus Patricia2, ,Beckers Johannes235,Wolf Eckhard4,Gailus‐Durner Valerie2,Fuchs Helmut2,Hrabe de Angelis Martin235,Ather Jennifer L.6,Poynter Matthew E.6,Krementsov Dimitry N.1ORCID

Affiliation:

1. Department of Biomedical and Health Sciences University of Vermont Burlington Vermont USA

2. Institute of Experimental Genetics and German Mouse Clinic Helmholtz Zentrum München Neuherberg Germany

3. German Center for Diabetes Research (DZD) Neuherberg Germany

4. Institute of Molecular Animal Breeding and Biotechnology, Gene Center Ludwig‐Maximilians‐University München Munich Germany

5. TUM School of Life Sciences Technische Universität München Freising Germany

6. Department of Medicine University of Vermont Burlington Vermont USA

Abstract

AbstractObesity is a global health problem characterized by excessive fat accumulation, driven by adipogenesis and lipid accumulation. Long non‐coding RNAs (lncRNAs) have recently been implicated in regulating adipogenesis and adipose tissue function. Mouse lncRNA U90926 was previously identified as a repressor of in vitro adipogenesis in 3T3‐L1 preadipocytes. Consequently, we hypothesized that, in vivo, U90926 may repress adipogenesis, and hence its deletion would increase weight gain and adiposity. We tested the hypothesis by applying U90926‐deficient (U9‐KO) mice to a high‐throughput phenotyping pipeline. Compared with WT, U9‐KO mice showed no major differences across a wide range of behavioral, neurological, and other physiological parameters. In mice fed a standard diet, we have found no differences in obesity‐related phenotypes, including weight gain, fat mass, and plasma concentrations of glucose, insulin, triglycerides, and free fatty acids, in U9‐KO mice compared to WT. U90926 deficiency lacked a major effect on white adipose tissue morphology and gene expression profile. Furthermore, in mice fed a high‐fat diet, we found increased expression of U90926 in adipose tissue stromal vascular cell fraction, yet observed no effect of U90926 deficiency on weight gain, fat mass, adipogenesis marker expression, and immune cell infiltration into the adipose tissue. These data suggest that the U90926 lacks an essential role in obesity‐related phenotypes and adipose tissue biology in vivo.

Publisher

Wiley

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