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

Author:

Klabunde Björn,Wesener André,Bertrams Wilhelm,Beinborn Isabell,Paczia Nicole,Surmann Kristin,Blankenburg Sascha,Wilhelm JochenORCID,Serrania Javier,Knoops Kèvin,Elsayed Eslam M.,Laakmann Katrin,Jung Anna Lena,Kirschbaum Andreas,Hammerschmidt SvenORCID,Alshaar Belal,Gisch NicolasORCID,Abu Mraheil Mobarak,Becker AnkeORCID,Völker UweORCID,Vollmeister EvelynORCID,Benedikter Birke J.ORCID,Schmeck BerndORCID

Abstract

AbstractLower 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+ 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+. Knockdown of NAD+ salvage enzymes (NAMPT, NMNAT1) increased bacterial replication. NAD+ treatment of Spn inhibited its growth while growth of other respiratory pathogens improved. Boosting NAD+ production increased NAD+ levels in immortalized and primary cells and decreased bacterial replication upon infection. NAD+ treatment of Spn dysregulated the bacterial metabolism and reduced intrabacterial ATP. Enhancing the bacterial ATP metabolism abolished the antibacterial effect of NAD+. Thus, we identified the NAD+ salvage pathway as an antibacterial pathway in Spn infections, predicting an antibacterial mechanism of NAD+.

Funder

Bundesministerium für Bildung und Forschung

Deutsche Forschungsgemeinschaft

Von-Behring-Röntgen-Stiftung

Hessisches Ministerium für Wissenschaft und Kunst

Publisher

Springer Science and Business Media LLC

Subject

General Physics and Astronomy,General Biochemistry, Genetics and Molecular Biology,General Chemistry,Multidisciplinary

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