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Merck

Oat-Derived β-Glucans Induced Trained Immunity Through Metabolic Reprogramming.

Inflammation (2020-03-15)
Wei Pan, Shanshan Hao, Mingxuan Zheng, Danhong Lin, Pengfei Jiang, Jinxiu Zhao, Hongli Shi, Xiaoying Yang, Xiangyang Li, Yinghua Yu
RESUMEN

Trained immunity has been recently identified in innate immune cells, which undergo long-term epigenetic and metabolic reprogramming after exposure to pathogens for protection from secondary infections. (1, 3)/(1, 6)-β-glucan derived from fungi can induce potent trained immunity; however, the effect of (1, 3)/(1, 4)-β-glucan (rich in dietary fiber oat) on trained immunity has not been reported. In the present study, two cell culture systems for trained immunity induction were validated in monocytes/macrophages from mouse bone myeloid and human THP-1 cells exposed to positive inducers of trained immunity, including β-glucan from Trametes versicolor or human-oxidized low-density lipoprotein. Primed with oat β-glucan, the mRNA expression and production of TNF-α and IL-6 significantly increased in response to re-stimulation of TLR-4/2 ligands. Moreover, the expression of several key enzymes in glycolytic pathway and tricarboxylic acid cycle was significantly upregulated. In addition, inhibiting these enzymes decreased the production of TNF-α and IL-6 boosted by oat β-glucan. These results show that oat β-glucan induces trained immunity through metabolic reprogramming. This provides important evidence that dietary fiber can maintain the long-term responsiveness of the innate immune system, which may benefit for prevention of infectious diseases or cancers.

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Sigma-Aldrich
2-Desoxi-D-glucosa, ≥98% (GC), crystalline
Sigma-Aldrich
Diethyl butylmalonate, 99%