GIPR Signaling in Immune Cells Maintains Metabolically Beneficial Type 2 Immune Responses in the White Fat From Obese Mice

Irina Efimova; Inbar Steinberg; Isabel Zvibel; Anat Neumann; Dana Fernanda Mantelmacher; Daniel J Drucker; Sigal Fishman; Chen Varol

doi:10.3389/fimmu.2021.643144

GIPR Signaling in Immune Cells Maintains Metabolically Beneficial Type 2 Immune Responses in the White Fat From Obese Mice

Front Immunol. 2021 Feb 25:12:643144. doi: 10.3389/fimmu.2021.643144. eCollection 2021.

Authors

Irina Efimova^{1

2}, Inbar Steinberg^{1

2}, Isabel Zvibel¹, Anat Neumann^{1

2}, Dana Fernanda Mantelmacher¹, Daniel J Drucker³, Sigal Fishman¹, Chen Varol^{1

2}

Affiliations

¹ The Research Center for Digestive Tract and Liver Diseases, Tel-Aviv Sourasky Medical Center Affiliated to Tel-Aviv University, Tel Aviv, Israel.
² Department of Clinical Microbiology and Immunology, Sackler School of Medicine, Tel-Aviv University, Tel-Aviv, Israel.
³ The Lunenfeld-Tanenbaum Research Institute, Mount Sinai Hospital, University of Toronto, Toronto, ON, Canada.

Abstract

Glucose-dependent insulinotropic polypeptide (GIP) communicates information on energy availability from the gut to peripheral tissues. Disruption of its signaling in myeloid immune cells during high-fat diet (HFD)-induced obesity impairs energy homeostasis due to the unrestrained metabolically deleterious actions of S100A8/A9 alarmin. White adipose tissue (WAT) type 2 immune cell networks are important for maintaining metabolic and energy homeostasis and limiting obesity-induced inflammation. Nevertheless, the consequences of losing immune cell GIP receptor (GIPR) signaling on type 2 immunity in WAT remains unknown. Bone marrow (BM) chimerism was used to generate mice with GIPR (Gipr^-/- BM) and GIPR/S100A8/A9 (Gipr^-/- /S100a9^-/- BM) deletion in immune cells. These mice were subjected to short (5 weeks) and progressive (14 weeks) HFD regimens. GIPR-deficiency was also targeted to myeloid cells by crossing Gipr^fl/fl mice and Lyz2^cre/+ mice (LysM^ΔGipr ). Under both short and progressive HFD regimens, Gipr^-/- BM mice exhibited altered expression of key type 2 immune cytokines in the epididymal visceral WAT (epiWAT), but not in subcutaneous inguinal WAT. This was further linked to declined representation of type 2 immune cells in epiWAT, such as group 2 innate lymphoid cells (ILC2), eosinophils, and FOXP3⁺ regulatory T cells (Tregs). Co-deletion of S100A8/A9 in Gipr^-/- immune cells reversed the impairment of type 2 cytokine expression in epiWAT, suggesting a mechanistic role for this alarmin in type 2 immune suppression. LysM^ΔGipr mice on HFD also displayed altered expression of type 2 immune mediators, highlighting that GIPR-deficiency in myeloid immune cells is responsible for the impairment of type 2 immune networks. Finally, abrogated GIPR signaling in immune cells also affected adipocyte fraction cells, inducing their increased production of the beiging interfering cytokine IL-10 and stress- related type 2 cytokine IL-13. Collectively, these findings attribute an important role for GIPR in myeloid immune cells in supporting WAT type 2 immunity.

Keywords: S100A8/A9; glucose-dependent insulinotropic polypeptide receptor; obesity; type 2 immunity; white adipose tissue.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Adipose Tissue, White / immunology*
Adipose Tissue, White / metabolism
Animals
Calgranulin A / physiology
Calgranulin B / physiology
Diet, High-Fat
Lymphocytes / immunology*
Male
Mice
Mice, Inbred C57BL
Mice, Obese
Obesity / immunology*
Receptors, Gastrointestinal Hormone / physiology*
Signal Transduction / physiology
Thermogenesis

Substances

Calgranulin A
Calgranulin B
Receptors, Gastrointestinal Hormone
S100A9 protein, mouse
S100a8 protein, mouse
gastric inhibitory polypeptide receptor

Grants and funding

154321/CIHR/Canada