Estrogen Regulates Sex-specific Localization of Regulatory T Cells in Adipose Tissue of Obese Female Mice

Overview

Journal PLoS One

Specialties General Medicine
Science

Date 2020 Apr 3

PMID 32240221

Citations 21

Authors

Akari Ishikawa

Tsutomu Wada

Sanshiro Nishimura

Tetsuo Ito

Akira Okekawa

Yasuhiro Onogi

Eri Watanabe

Azusa Sameshima

Tomoko Tanaka

Hiroshi Tsuneki

Shigeru Saito

Toshiyasu Sasaoka

Affiliations

Soon will be listed here.

Abstract

Regulatory T cells (Treg) play essential roles in maintaining immune homeostasis. Resident Treg in visceral adipose tissue (VAT-Treg) decrease in male obese mice, which leads to the development of obesity-associated chronic inflammations and insulin resistance. Although gender differences in immune responses have been reported, the effects of the difference in metabolic environment on VAT-Treg are unclear. We investigated the localization of VAT-Treg in female mice in comparison with that in male mice. On a high-fat diet (HFD), VAT-Treg decreased in male mice but increased in female mice. The increase was abolished in ovariectomized and HFD-fed mice, but was restored by estrogen supplementation. The IL33 receptor ST2, which is important for the localization and maturation of VAT-Treg in males, was reduced in CD4+CD25+ T cells isolated from gonadal fat of obese mice of both genders, suggesting that a different system exists for VAT-Treg localization in females. Extensive analysis of chemokine expression in gonadal fat and adipose CD4+CD25+T cells revealed several chemokine signals related to female-specific VAT-Treg accumulation such as CCL24, CCR6, and CXCR3. Taken together, the current study demonstrated sexual dimorphism in VAT-Treg localization in obese mice. Estrogen may attenuate obesity-associated chronic inflammation partly through altering chemokine-related VAT-Treg localization in females.

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