Eosinophils regulate adipose tissue inflammation and sustain physical and immunological fitness in old age

炎症 脂肪组织 老化 全身炎症 嗜酸性粒细胞 免疫衰老 免疫系统 免疫学 平衡 医学 生物 内科学 哮喘
作者
Daniel Brigger,Carsten Riether,Robin van Brummelen,Kira I. Mosher,Alicia Shiu,Zhaoqing Ding,Noemi Zbären,Philippe Gasser,Pascal Guntern,Hanadie Yousef,Joseph M. Castellano,Federico Storni,Neill R. Graff‐Radford,Markus Britschgi,Denis Grandgirard,Magdalena Hinterbrandner,Mark Siegrist,Norman Moullan,Willy Hofstetter,Stephen L. Leib,Peter M. Villiger,Johan Auwerx,Saul Villeda,Tony Wyss‐Coray,Mario Noti,Alexander Eggel
出处
期刊:Nature metabolism [Springer Nature]
卷期号:2 (8): 688-702 被引量:76
标识
DOI:10.1038/s42255-020-0228-3
摘要

Adipose tissue eosinophils (ATEs) are important in the control of obesity-associated inflammation and metabolic disease. However, the way in which ageing impacts the regulatory role of ATEs remains unknown. Here, we show that ATEs undergo major age-related changes in distribution and function associated with impaired adipose tissue homeostasis and systemic low-grade inflammation in both humans and mice. We find that exposure to a young systemic environment partially restores ATE distribution in aged parabionts and reduces adipose tissue inflammation. Approaches to restore ATE distribution using adoptive transfer of eosinophils from young mice into aged recipients proved sufficient to dampen age-related local and systemic low-grade inflammation. Importantly, restoration of a youthful systemic milieu by means of eosinophil transfers resulted in systemic rejuvenation of the aged host, manifesting in improved physical and immune fitness that was partially mediated by eosinophil-derived IL-4. Together, these findings support a critical function of adipose tissue as a source of pro-ageing factors and uncover a new role of eosinophils in promoting healthy ageing by sustaining adipose tissue homeostasis. Brigger et al. show that adipose tissue eosinophil dysfunction with age underpins physiological features of ageing, including global inflammation, loss of physical fitness and myeloid skewing. Eosinophils transferred from young to aged mice reversed these features and improved immunological fitness in old age, in part via IL-4.
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