Frontiers in Immunology (May 2018)

Distinct Housing Conditions Reveal a Major Impact of Adaptive Immunity on the Course of Obesity-Induced Type 2 Diabetes

  • Julia Sbierski-Kind,
  • Julia Sbierski-Kind,
  • Julia Sbierski-Kind,
  • Julia Sbierski-Kind,
  • Jonas Kath,
  • Jonas Kath,
  • Sebastian Brachs,
  • Sebastian Brachs,
  • Mathias Streitz,
  • Mathias Streitz,
  • Matthias G. von Herrath,
  • Matthias G. von Herrath,
  • Anja A. Kühl,
  • Anja A. Kühl,
  • Katharina Schmidt-Bleek,
  • Katharina Schmidt-Bleek,
  • Knut Mai,
  • Knut Mai,
  • Knut Mai,
  • Joachim Spranger,
  • Joachim Spranger,
  • Joachim Spranger,
  • Hans-Dieter Volk,
  • Hans-Dieter Volk

DOI
https://doi.org/10.3389/fimmu.2018.01069
Journal volume & issue
Vol. 9

Abstract

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Obesity is associated with adipose tissue inflammation, insulin resistance, and the development of type 2 diabetes (T2D). However, our knowledge is mostly based on conventional murine models and promising preclinical studies rarely translated into successful therapies. There is a growing awareness of the limitations of studies in laboratory mice, housed in abnormally hygienic specific pathogen-free (SPF) conditions, as relevant aspects of the human immune system remain unappreciated. Here, we assessed the impact of housing conditions on adaptive immunity and metabolic disease processes during high-fat diet (HFD). We therefore compared diet-induced obesity in SPF mice with those housed in non-SPF, so-called “antigen exposed” (AE) conditions. Surprisingly, AE mice fed a HFD maintained increased insulin levels to compensate for insulin resistance, which was reflected in islet hyperplasia and improved glucose tolerance compared to SPF mice. By contrast, we observed higher proportions of effector/memory T cell subsets in blood and liver of HFD AE mice accompanied by the development of non-alcoholic steatohepatitis-like liver pathology. Thus, our data demonstrate the impact of housing conditions on metabolic alterations. Studies in AE mice, in which physiological microbial exposure was restored, could provide a tool for revealing therapeutic targets for immune-based interventions for T2D patients.

Keywords