CD4+ T cells regulate glucose homeostasis independent of adipose tissue dysfunction in mice |
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| Authors: | Georg Brinker Janine Froeba Lilli Arndt Julia Braune Constance Hobusch Andreas Lindhorst Ingo Bechmann Martin Gericke |
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| Affiliation: | 1. Institute of Anatomy, Leipzig University, Leipzig, D-04103 Germany;2. Institute of Anatomy, Leipzig University, Leipzig, D-04103 Germany Institute of Anatomy and Cell Biology, Martin-Luther-University Halle-Wittenberg, Halle (Saale), D-06108 Germany;3. Institute of Anatomy and Cell Biology, Martin-Luther-University Halle-Wittenberg, Halle (Saale), D-06108 Germany |
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| Abstract: | Obesity is frequently associated with a chronic low-grade inflammation in the adipose tissue (AT) and impaired glucose homeostasis. Adipose tissue macrophages (ATMs) have been shown to accumulate in the inflamed AT either by means of recruitment from the blood or local proliferation. ATM proliferation and activation can be stimulated by TH2 cytokines, such as IL-4 and IL-13, suggesting involvement of CD4-positive T cells in ATM proliferation and activation. Furthermore, several studies have associated T cells to alterations in glucose metabolism. Therefore, we sought to examine a direct impact of CD4-positive T cells on ATM activation, ATM proliferation and glucose homeostasis using an in vivo depletion model. Surprisingly, CD4 depletion did not affect ATM activation, ATM proliferation, or insulin sensitivity. However, CD4 depletion led to a significant improvement of glucose tolerance. In line with this, we found moderate disturbances in pancreatic endocrine function following CD4 depletion. Hence, our data suggest that the effect on glucose metabolism observed after CD4 depletion might be mediated by organs other than AT and independent of AT inflammation. |
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| Keywords: | adipose tissue inflammation lymphocytes macrophages obesity |
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