| Literature DB >> 32103173 |
Ajithkumar Vasanthakumar1,2, David Chisanga3,4, Jonas Blume5,3, Renee Gloury5,3, Kara Britt6, Darren C Henstridge7, Yifan Zhan3,4, Santiago Valle Torres5, Sebastian Liene5,8, Nicholas Collins5, Enyuan Cao9, Tom Sidwell5,3, Chaoran Li10, Raul German Spallanzani10, Yang Liao3,4, Paul A Beavis6, Thomas Gebhardt5, Natalie Trevaskis9, Stephen L Nutt3,4, Jeffrey D Zajac11, Rachel A Davey11, Mark A Febbraio9, Diane Mathis10, Wei Shi3,12, Axel Kallies13,14.
Abstract
Adipose tissue is an energy store and a dynamic endocrine organ1,2. In particular, visceral adipose tissue (VAT) is critical for the regulation of systemic metabolism3,4. Impaired VAT function-for example, in obesity-is associated with insulin resistance and type 2 diabetes5,6. Regulatory T (Treg) cells that express the transcription factor FOXP3 are critical for limiting immune responses and suppressing tissue inflammation, including in the VAT7-9. Here we uncover pronounced sexual dimorphism in Treg cells in the VAT. Male VAT was enriched for Treg cells compared with female VAT, and Treg cells from male VAT were markedly different from their female counterparts in phenotype, transcriptional landscape and chromatin accessibility. Heightened inflammation in the male VAT facilitated the recruitment of Treg cells via the CCL2-CCR2 axis. Androgen regulated the differentiation of a unique IL-33-producing stromal cell population specific to the male VAT, which paralleled the local expansion of Treg cells. Sex hormones also regulated VAT inflammation, which shaped the transcriptional landscape of VAT-resident Treg cells in a BLIMP1 transcription factor-dependent manner. Overall, we find that sex-specific differences in Treg cells from VAT are determined by the tissue niche in a sex-hormone-dependent manner to limit adipose tissue inflammation.Entities:
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Year: 2020 PMID: 32103173 PMCID: PMC7241647 DOI: 10.1038/s41586-020-2040-3
Source DB: PubMed Journal: Nature ISSN: 0028-0836 Impact factor: 49.962