DsbA-L deficiency in T cells promotes diet-induced thermogenesis through suppressing IFN-γ production.
Haiyan ZhouXinyi PengJie HuLiwen WangHairong LuoJunyan ZhangYacheng ZhangGuobao LiYujiao JiJingjing ZhangJuli BaiMeilian LiuZhiguang ZhouFeng LiuPublished in: Nature communications (2021)
Adipose tissue-resident T cells have been recognized as a critical regulator of thermogenesis and energy expenditure, yet the underlying mechanisms remain unclear. Here, we show that high-fat diet (HFD) feeding greatly suppresses the expression of disulfide-bond A oxidoreductase-like protein (DsbA-L), a mitochondria-localized chaperone protein, in adipose-resident T cells, which correlates with reduced T cell mitochondrial function. T cell-specific knockout of DsbA-L enhances diet-induced thermogenesis in brown adipose tissue (BAT) and protects mice from HFD-induced obesity, hepatosteatosis, and insulin resistance. Mechanistically, DsbA-L deficiency in T cells reduces IFN-γ production and activates protein kinase A by reducing phosphodiesterase-4D expression, leading to increased BAT thermogenesis. Taken together, our study uncovers a mechanism by which T cells communicate with brown adipocytes to regulate BAT thermogenesis and whole-body energy homeostasis. Our findings highlight a therapeutic potential of targeting T cells for the treatment of over nutrition-induced obesity and its associated metabolic diseases.
Keyphrases
- amino acid
- adipose tissue
- high fat diet
- insulin resistance
- high fat diet induced
- poor prognosis
- polycystic ovary syndrome
- high glucose
- diabetic rats
- patient safety
- immune response
- protein kinase
- metabolic syndrome
- dendritic cells
- replacement therapy
- weight loss
- physical activity
- quality improvement
- type diabetes
- binding protein
- body mass index
- drug induced
- skeletal muscle
- cancer therapy
- cell death
- transcription factor
- long non coding rna
- endothelial cells
- emergency medicine
- heat shock