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NAD+ metabolism is a key modulator of bacterial respiratory epithelial infections

31

Citations

68

References

2023

Year

Abstract

Lower respiratory tract infections caused by Streptococcus pneumoniae (Spn) are a leading cause of death globally. Here we investigate the bronchial epithelial cellular response to Spn infection on a transcriptomic, proteomic and metabolic level. We found the NAD<sup>+</sup> salvage pathway to be dysregulated upon infection in a cell line model, primary human lung tissue and in vivo in rodents, leading to a reduced production of NAD<sup>+</sup>. Knockdown of NAD<sup>+</sup> salvage enzymes (NAMPT, NMNAT1) increased bacterial replication. NAD<sup>+</sup> treatment of Spn inhibited its growth while growth of other respiratory pathogens improved. Boosting NAD<sup>+</sup> production increased NAD<sup>+</sup> levels in immortalized and primary cells and decreased bacterial replication upon infection. NAD<sup>+</sup> treatment of Spn dysregulated the bacterial metabolism and reduced intrabacterial ATP. Enhancing the bacterial ATP metabolism abolished the antibacterial effect of NAD<sup>+</sup>. Thus, we identified the NAD<sup>+</sup> salvage pathway as an antibacterial pathway in Spn infections, predicting an antibacterial mechanism of NAD<sup>+</sup>.

References

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