Author
Listed:
- Tuo Deng
(Center for Bioenergetics, Houston Methodist Research Institute, Weill Cornell Medical College
Diabetes Center, Institute of Metabolism and Endocrinology, The Second Xiangya Hospital and Key Laboratory of Diabetes Immunology (Central South University), Ministry of Education)
- Joey Liu
(The Diabetes and Metabolism Research Center, Diabetes and Metabolism, The Ohio State University)
- Yanru Deng
(Center for Bioenergetics, Houston Methodist Research Institute, Weill Cornell Medical College)
- Laurie Minze
(Immunobiology and Transplantation Research, Houston Methodist Research Institute, Texas Medical Center)
- Xiang Xiao
(Immunobiology and Transplantation Research, Houston Methodist Research Institute, Texas Medical Center)
- Valerie Wright
(The Diabetes and Metabolism Research Center, Diabetes and Metabolism, The Ohio State University)
- Richeng Yu
(Center for Bioenergetics, Houston Methodist Research Institute, Weill Cornell Medical College
Guizhou Provincial People's Hospital)
- Xian C. Li
(Immunobiology and Transplantation Research, Houston Methodist Research Institute, Texas Medical Center)
- Alecia Blaszczak
(The Diabetes and Metabolism Research Center, Diabetes and Metabolism, The Ohio State University
Medical Scientist Training Program and Biomedical Sciences Graduate Program, The Ohio State University)
- Stephen Bergin
(The Comprehensive Cancer Center–Arthur G. James Cancer Hospital and Richard J. Solove Research Institute, The Ohio State University
Medical Scientist Training Program and Biomedical Sciences Graduate Program, The Ohio State University)
- David DiSilvestro
(The Diabetes and Metabolism Research Center, Diabetes and Metabolism, The Ohio State University)
- Ryan Judd
(Medical Scientist Training Program and Biomedical Sciences Graduate Program, The Ohio State University)
- David Bradley
(The Diabetes and Metabolism Research Center, Diabetes and Metabolism, The Ohio State University)
- Michael Caligiuri
(Medical Scientist Training Program and Biomedical Sciences Graduate Program, The Ohio State University)
- Christopher J. Lyon
(Center for Bioenergetics, Houston Methodist Research Institute, Weill Cornell Medical College
Present address: Virginia G. Piper Biodesign Center for Personalized Diagnostics, The Biodesign Institute, Arizona State University, Tempe, Arizona 85287, USA)
- Willa A. Hsueh
(The Diabetes and Metabolism Research Center, Diabetes and Metabolism, The Ohio State University)
Abstract
Obesity leads to a switch in subsets of CD4+ T cell in adipose tissue, characterized by an increase in IFNγ producing Th1 cells and a decrease in anti-inflammatory regulatory T (Treg) cells, which impairs systemic insulin sensitivity. What signals these changes is unknown. Herein we demonstrate that genetic deficiency of adipocyte MHCII decreases adipose IFNγ expression and increases adipose Treg abundance in obese mice, leading to reduced obesity-induced adipose inflammation and reduced insulin resistance without affecting weight gain. The preserved insulin sensitivity of high fat diet (HFD)-fed adipocyte-specific MHCII knockout (aMHCII−/−) mice was substantially attenuated by adipose-specific Treg ablation. Adipocytes of aMHCII−/− mice exhibit decreased capacity to stimulate IFNγ production in Th1 cells, whereas HFD-fed IFNγR1−/− mice were more insulin sensitive and had similarly high levels of Tregs in adipose tissue as aMHCII−/− mice. We further show that IFNγ strongly inhibits IL-33 effects to promote adipose Treg proliferation. Our results identify MHCII in adipocyte as a critical determinant of the obesity-induced adipose T cell subset switch and insulin resistance.
Suggested Citation
Tuo Deng & Joey Liu & Yanru Deng & Laurie Minze & Xiang Xiao & Valerie Wright & Richeng Yu & Xian C. Li & Alecia Blaszczak & Stephen Bergin & David DiSilvestro & Ryan Judd & David Bradley & Michael Ca, 2017.
"Adipocyte adaptive immunity mediates diet-induced adipose inflammation and insulin resistance by decreasing adipose Treg cells,"
Nature Communications, Nature, vol. 8(1), pages 1-11, August.
Handle:
RePEc:nat:natcom:v:8:y:2017:i:1:d:10.1038_ncomms15725
DOI: 10.1038/ncomms15725
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