NAD(H) homeostasis underlies host protection mediated by glycolytic myeloid cells in tuberculosis.
Hayden T PaclKrishna C ChintaVineel P ReddySajid NadeemRitesh R SevalkarKievershen NarganKapongo LumambaThrenesan NaidooJoel N GlasgowAnupam AgarwalAdrie J C SteynPublished in: Nature communications (2023)
Mycobacterium tuberculosis (Mtb) disrupts glycolytic flux in infected myeloid cells through an unclear mechanism. Flux through the glycolytic pathway in myeloid cells is inextricably linked to the availability of NAD + , which is maintained by NAD + salvage and lactate metabolism. Using lung tissue from tuberculosis (TB) patients and myeloid deficient LDHA (Ldha LysM-/- ) mice, we demonstrate that glycolysis in myeloid cells is essential for protective immunity in TB. Glycolytic myeloid cells are essential for the early recruitment of multiple classes of immune cells and IFNγ-mediated protection. We identify NAD + depletion as central to the glycolytic inhibition caused by Mtb. Lastly, we show that the NAD + precursor nicotinamide exerts a host-dependent, antimycobacterial effect, and that nicotinamide prophylaxis and treatment reduce Mtb lung burden in mice. These findings provide insight into how Mtb alters host metabolism through perturbation of NAD(H) homeostasis and reprogramming of glycolysis, highlighting this pathway as a potential therapeutic target.
Keyphrases
- mycobacterium tuberculosis
- induced apoptosis
- pulmonary tuberculosis
- cell cycle arrest
- dendritic cells
- acute myeloid leukemia
- bone marrow
- oxidative stress
- emergency department
- signaling pathway
- cell death
- immune response
- adipose tissue
- cell proliferation
- risk assessment
- climate change
- ejection fraction
- patient reported outcomes
- skeletal muscle
- peritoneal dialysis
- human immunodeficiency virus
- electronic health record
- replacement therapy