Send to

Choose Destination
Mol Metab. 2016 May 14;5(7):480-490. doi: 10.1016/j.molmet.2016.05.005. eCollection 2016 Jul.

Lipodystrophy and severe metabolic dysfunction in mice with adipose tissue-specific insulin receptor ablation.

Author information

Department of Physiology & Biophysics, University of Illinois at Chicago, Chicago, IL, USA.
Department of Molecular & Integrative Physiology, University of Michigan, Ann Arbor, MI, USA.
Department of Kinesiology and Nutrition, University of Illinois at Chicago, Chicago, IL, USA.
Department of Physiology & Biophysics, University of Illinois at Chicago, Chicago, IL, USA. Electronic address:



Insulin signaling plays pivotal roles in the development and metabolism of many tissues and cell types. A previous study demonstrated that ablation of insulin receptor (IR) with aP2-Cre markedly reduced adipose tissues mass and protected mice from obesity. However, multiple studies have demonstrated widespread non-adipocyte recombination of floxed alleles in aP2-Cre mice. These findings underscore the need to re-evaluate the role of IR in adipocyte and systemic metabolism with a more adipose tissue-specific Cre mouse line.


We generated and phenotyped a new adipose tissue-specific IR mouse model using the adipose tissue-specific Adipoq-Cre line.


Here we show that the Adipoq-Cre-mediated IR KO in mice leads to lipodystrophy and metabolic dysfunction, which is in stark contrast to the previous study. In contrast to white adipocytes, absence of insulin signaling does not affect development of marrow and brown adipocytes, but instead is required for lipid accumulation particularly for the marrow adipocytes. Lipodystrophic IR KO mice have profound insulin resistance, hyperglycemia, organomegaly, and impaired adipokine secretion.


Our results demonstrate differential roles for insulin signaling for white, brown, and marrow adipocyte development and metabolic regulation.


Brown adipose tissue; Insulin signaling; Lipodystrophy; Marrow adipose tissue; White adipose tissue

Supplemental Content

Full text links

Icon for Elsevier Science Icon for PubMed Central
Loading ...
Support Center