Novel Grb14-Mediated Cross Talk between Insulin and p62/Nrf2 Pathways Regulates Liver Lipogenesis and Selective Insulin Resistance

Lucie Popineau; Lucille Morzyglod; Nadège Carré; Michèle Caüzac; Pascale Bossard; Carina Prip-Buus; Véronique Lenoir; Bruno Ragazzon; Véronique Fauveau; Lorenne Robert; Sandra Guilmeau; Catherine Postic; Masaaki Komatsu; François Canonne-Hergaux; Hervé Guillou; Anne-Françoise Burnol

doi:10.1128/MCB.00170-16

Novel Grb14-Mediated Cross Talk between Insulin and p62/Nrf2 Pathways Regulates Liver Lipogenesis and Selective Insulin Resistance

Mol Cell Biol. 2016 Jul 29;36(16):2168-81. doi: 10.1128/MCB.00170-16. Print 2016 Aug 15.

Authors

Lucie Popineau¹, Lucille Morzyglod¹, Nadège Carré¹, Michèle Caüzac¹, Pascale Bossard¹, Carina Prip-Buus¹, Véronique Lenoir¹, Bruno Ragazzon¹, Véronique Fauveau¹, Lorenne Robert², Sandra Guilmeau¹, Catherine Postic¹, Masaaki Komatsu³, François Canonne-Hergaux², Hervé Guillou⁴, Anne-Françoise Burnol⁵

Affiliations

¹ INSERM, U1016, Institut Cochin, Paris, France CNRS, UMR8104, Paris, France Université Paris Descartes, Sorbonne Paris Cité, Paris, France.
² INSERM U1043, Toulouse, France CNRS, unité 5282, Toulouse, France IRSD, INSERM, INRA, ENVT, UPS, Toulouse, France.
³ Protein Metabolism Project, Tokyo Metropolitan Institute of Medical Science, Tokyo, Japan.
⁴ Institut National de la Recherche Agronomique, ToxAlim Unité Mixte de Recherche 1331, Toulouse, France Université de Toulouse, INP, UPS, ToxAlim, Toulouse, France.
⁵ INSERM, U1016, Institut Cochin, Paris, France CNRS, UMR8104, Paris, France Université Paris Descartes, Sorbonne Paris Cité, Paris, France anne-francoise.burnol@inserm.fr.

Abstract

A long-standing paradox in the pathophysiology of metabolic diseases is the selective insulin resistance of the liver. It is characterized by a blunted action of insulin to reduce glucose production, contributing to hyperglycemia, while de novo lipogenesis remains insulin sensitive, participating in turn to hepatic steatosis onset. The underlying molecular bases of this conundrum are not yet fully understood. Here, we established a model of selective insulin resistance in mice by silencing an inhibitor of insulin receptor catalytic activity, the growth factor receptor binding protein 14 (Grb14) in liver. Indeed, Grb14 knockdown enhanced hepatic insulin signaling but also dramatically inhibited de novo fatty acid synthesis. In the liver of obese and insulin-resistant mice, downregulation of Grb14 markedly decreased blood glucose and improved liver steatosis. Mechanistic analyses showed that upon Grb14 knockdown, the release of p62/sqstm1, a partner of Grb14, activated the transcription factor nuclear factor erythroid-2-related factor 2 (Nrf2), which in turn repressed the lipogenic nuclear liver X receptor (LXR). Our study reveals that Grb14 acts as a new signaling node that regulates lipogenesis and modulates insulin sensitivity in the liver by acting at a crossroad between the insulin receptor and the p62-Nrf2-LXR signaling pathways.

MeSH terms

Adaptor Proteins, Signal Transducing
Animals
Cyclin-Dependent Kinase Inhibitor p16 / metabolism
Gene Expression Regulation
Gene Knockdown Techniques
Insulin Resistance*
Lipogenesis*
Liver / cytology
Liver / metabolism*
Liver X Receptors / metabolism
Mice
NF-E2-Related Factor 2 / metabolism
Proteins / genetics*
Proteins / metabolism
Receptor, Insulin / metabolism
Signal Transduction*

Substances

Adaptor Proteins, Signal Transducing
Cyclin-Dependent Kinase Inhibitor p16
Grb14 protein, mouse
Liver X Receptors
NF-E2-Related Factor 2
Nfe2l2 protein, mouse
Proteins
Receptor, Insulin

Grants and funding

Renaud Dentin was the recipient of Agence Nationale de la Recherche (ANR) grant ANR-09-JCJC-0057.