Literature DB >> 29457786

Intracellular lipid metabolism impairs β cell compensation during diet-induced obesity.

Risheng Ye1,2, Ruth Gordillo1, Mengle Shao1, Toshiharu Onodera1, Zhe Chen1,3, Shiuhwei Chen1, Xiaoli Lin1, Jeffrey A SoRelle3, Xiaohong Li3, Miao Tang3, Mark P Keller4, Regina Kuliawat5, Alan D Attie4, Rana K Gupta1, William L Holland1, Bruce Beutler3, Joachim Herz6,7, Philipp E Scherer1.   

Abstract

The compensatory proliferation of insulin-producing β cells is critical to maintaining glucose homeostasis at the early stage of type 2 diabetes. Failure of β cells to proliferate results in hyperglycemia and insulin dependence in patients. To understand the effect of the interplay between β cell compensation and lipid metabolism upon obesity and peripheral insulin resistance, we eliminated LDL receptor-related protein 1 (LRP1), a pleiotropic mediator of cholesterol, insulin, energy metabolism, and other cellular processes, in β cells. Upon high-fat diet exposure, LRP1 ablation significantly impaired insulin secretion and proliferation of β cells. The diminished insulin signaling was partly contributed to by the hypersensitivity to glucose-induced, Ca2+-dependent activation of Erk and the mTORC1 effector p85 S6K1. Surprisingly, in LRP1-deficient islets, lipotoxic sphingolipids were mitigated by improved lipid metabolism, mediated at least in part by the master transcriptional regulator PPARγ2. Acute overexpression of PPARγ2 in β cells impaired insulin signaling and insulin secretion. Elimination of Apbb2, a functional regulator of LRP1 cytoplasmic domain, also impaired β cell function in a similar fashion. In summary, our results uncover the double-edged effects of intracellular lipid metabolism on β cell function and viability in obesity and type 2 diabetes and highlight LRP1 as an essential regulator of these processes.

Entities:  

Keywords:  Beta cells; Diabetes; Endocrinology; Metabolism; Obesity

Mesh:

Substances:

Year:  2018        PMID: 29457786      PMCID: PMC5824868          DOI: 10.1172/JCI97702

Source DB:  PubMed          Journal:  J Clin Invest        ISSN: 0021-9738            Impact factor:   14.808


  66 in total

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