Succinate and inosine coordinate innate immune response to bacterial infection

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Abstract

Macrophages restrict bacterial infection partly by stimulating phagocytosis and partly by stimulating release of cytokines and complement components. Here, we treat macrophages with LPS and a bacterial pathogen, and demonstrate that expression of cytokine IL-1? and bacterial phagocytosis increase to a transient peak 8 to 12 h post-Treatment, while expression of complement component 3 (C3) continues to rise for 24 h post-Treatment. Metabolomic analysis suggests a correlation between the cellular concentrations of succinate and IL-1? and of inosine and C3. This may involve a regulatory feedback mechanism, whereby succinate stimulates and inosine inhibits HIF-1? through their competitive interactions with prolyl hydroxylase. Furthermore, increased level of inosine in LPS-stimulated macrophages is linked to accumulation of adenosine monophosphate and that exogenous inosine improves the survival of bacterial pathogen-infected mice and tilapia. The implications of these data suggests potential therapeutic tools to prevent, manage or treat bacterial infections.

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APA

Jiang, M., Chen, Z., Li, H., Zhang, T., Yang, M., Peng, X., & Peng, B. (2022). Succinate and inosine coordinate innate immune response to bacterial infection. PLoS Pathogens, 18(8). https://doi.org/10.1371/journal.ppat.1010796

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