Intermuscular and perimuscular fat expansion in obesity correlates with skeletal muscle T cell and macrophage infiltration and insulin resistance

IM Khan, XYD Perrard, G Brunner, H Lui… - International journal of …, 2015 - nature.com
IM Khan, XYD Perrard, G Brunner, H Lui, LM Sparks, SR Smith, X Wang, ZZ Shi, DE Lewis…
International journal of obesity, 2015nature.com
Results: Macrophage and T-cell markers were upregulated in SM of obese compared with
lean humans. SM of obese mice had higher expression of inflammatory cytokines, with
macrophages increasing by 2 weeks on HFD and T cells increasing by 8 weeks. The
immune cells were localized in EMAT. Micro-CT revealed that EMAT expansion in obese
mice correlated with T-cell infiltration and insulin resistance. Deficiency or neutralization of
CD11a reduced T-cell accumulation in SM of obese mice. T cells polarized into a …
Results:
Macrophage and T-cell markers were upregulated in SM of obese compared with lean humans. SM of obese mice had higher expression of inflammatory cytokines, with macrophages increasing by 2 weeks on HFD and T cells increasing by 8 weeks. The immune cells were localized in EMAT. Micro-CT revealed that EMAT expansion in obese mice correlated with T-cell infiltration and insulin resistance. Deficiency or neutralization of CD11a reduced T-cell accumulation in SM of obese mice. T cells polarized into a proinflammatory T H 1 phenotype, with increased STAT1 phosphorylation in SM of obese mice. In vivo inhibition of JAK/STAT pathway with baricitinib reduced T-cell numbers and activation markers in SM and adipose tissue and improved insulin resistance in obese mice.
Conclusions:
Obesity-induced expansion of EMAT in SM was associated with accumulation and proinflammatory polarization of T cells, which may regulate SM metabolic functions through paracrine mechanisms. Obesity-associated SM ‘adiposopathy'may thus have an important role in the development of insulin resistance and inflammation.
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