Obesity accelerates T cell senescence in murine visceral adipose tissue
Kohsuke Shirakawa, Xiaoxiang Yan, Ken Shinmura, Jin Endo, Masaharu Kataoka, Yoshinori Katsumata, Tsunehisa Yamamoto, Atsushi Anzai, Sarasa Isobe, Naohiro Yoshida, Hiroshi Itoh, Ichiro Manabe, Miho Sekai, Yoko Hamazaki, Keiichi Fukuda, Nagahiro Minato, Motoaki Sano
Kohsuke Shirakawa, Xiaoxiang Yan, Ken Shinmura, Jin Endo, Masaharu Kataoka, Yoshinori Katsumata, Tsunehisa Yamamoto, Atsushi Anzai, Sarasa Isobe, Naohiro Yoshida, Hiroshi Itoh, Ichiro Manabe, Miho Sekai, Yoko Hamazaki, Keiichi Fukuda, Nagahiro Minato, Motoaki Sano
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Research Article Immunology Metabolism

Obesity accelerates T cell senescence in murine visceral adipose tissue

Abstract

Chronic inflammation in visceral adipose tissue (VAT) precipitates the development of cardiometabolic disorders. Although changes in T cell function associated with visceral obesity are thought to affect chronic VAT inflammation, the specific features of these changes remain elusive. Here, we have determined that a high-fat diet (HFD) caused a preferential increase and accumulation of CD44hiCD62LloCD4+ T cells that constitutively express PD-1 and CD153 in a B cell–dependent manner in VAT. These cells possessed characteristics of cellular senescence and showed a strong activation of Spp1 (encoding osteopontin [OPN]) in VAT. Upon T cell receptor stimulation, these T cells also produced large amounts of OPN in a PD-1–resistant manner in vitro. The features of CD153+PD-1+CD44hiCD4+ T cells were highly reminiscent of senescence-associated CD4+ T cells that normally increase with age. Adoptive transfer of CD153+PD-1+CD44hiCD4+ T cells from HFD-fed WT, but not Spp1-deficient, mice into the VAT of lean mice fed a normal diet recapitulated the essential features of VAT inflammation and insulin resistance. Our results demonstrate that a distinct CD153+PD-1+CD44hiCD4+ T cell population that accumulates in the VAT of HFD-fed obese mice causes VAT inflammation by producing large amounts of OPN. This finding suggests a link between visceral adiposity and immune aging.

Authors

Kohsuke Shirakawa, Xiaoxiang Yan, Ken Shinmura, Jin Endo, Masaharu Kataoka, Yoshinori Katsumata, Tsunehisa Yamamoto, Atsushi Anzai, Sarasa Isobe, Naohiro Yoshida, Hiroshi Itoh, Ichiro Manabe, Miho Sekai, Yoko Hamazaki, Keiichi Fukuda, Nagahiro Minato, Motoaki Sano

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Figure 9

CD153+PD-1+CD4+ T cells cause VAT inflammation and insulin resistance by secreting OPN.

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CD153+PD-1+CD4+ T cells cause VAT inflammation and insulin resistance by...
(AD) Splenic CD153+PD-1+CD4+ T cells were separately isolated from HFD-fed WT and Spp1–/– mice, respectively. Cells (1 × 105) were transferred directly into VAT of individual recipient ND-fed lean mice 3 times per week for 2 weeks, starting at 18 weeks of age. ND-fed lean mice receiving vehicle (thermoreversible gelation polymer) were used as the control group. (A) Analyses of Spp1, Ifng, Tnfa, and Il6 expression by real-time PCR in VAT of recipient mice (n = 5 mice per group). (B) Analyses of CD11chiCD206lo macrophages and CD11cloCD206hi macrophage ratios in VAT of recipient mice (n = 5 mice per group). (C) Analyses of serum OPN and IgG concentrations in recipient mice (n = 6 mice per group). (D) Effects of adoptive transfer of control reagent or CD153+PD-1+CD4+ T cells from WT or Spp1–/– mice fed an HFD as determined by OGTT and ITT (n = 10 mice per group). *P < 0.05, for WT CD153+PD-1+CD4+ T cells versus vehicle (n = 10 mice per group). Data represent the mean ± SEM. *P < 0.05 and ***P < 0.0001, by ANOVA followed by post hoc Bonferroni tests