Abstract
Macrophages are indispensable immune cells tasked at eliminating intracellular pathogens. Mycobacterium tuberculosis (Mtb), one of the most virulent intracellular bacterial pathogens known to man, infects and resides within macrophages. While macrophages can be provoked by extracellular stimuli to inhibit and kill Mtb bacilli, these host defense mechanisms can be blocked by limiting nutritional metabolites, such as amino acids. The amino acid L-arginine has been well described to enhance immune function, especially in the context of driving macrophage nitric oxide (NO) production in mice. In this study, we aimed to establish the necessity of L-arginine on anti-Mtb macrophage function independent of NO. Utilizing an in vitro system, we identified that macrophages relied on NO for only half of their L-arginine-mediated host defenses and this L-arginine-mediated defense in the absence of NO was associated with enhanced macrophage numbers and viability. Additionally, we observed macrophage glycolysis to be driven by both L-arginine and mechanistic target of rapamycin (mTOR), and inhibition of glycolysis or mTOR reduced macrophage control of Mtb as well as macrophage number and viability in the presence of L-arginine. Our data underscore L-arginine as an essential nutrient for macrophage function, not only by fueling anti-mycobacterial NO production, but also as a central regulator of macrophage metabolism and additional host defense mechanisms.
Highlights
Mycobacterium tuberculosis (Mtb), the causative agent of tuberculosis, is a persistent pathogen which continues to plague a quarter of the world’s population despite the availability of antibiotics [1, 2]
When Mtb was cultured without macrophages, there was no effect of L-arginine or L-citrulline on Mtb growth, indicating the amino acids were acting on macrophages rather than directly inhibiting Mtb growth (Figure S1E)
Analysis over time demonstrated that L-arginine or Lcitrulline primarily resulted in bacteriostatic control of Mtb by macrophages (Figure S1F)
Summary
Mycobacterium tuberculosis (Mtb), the causative agent of tuberculosis, is a persistent pathogen which continues to plague a quarter of the world’s population despite the availability of antibiotics [1, 2]. Peripheral immune cells, especially T cells and NK cells that produce interferon (IFN)-g, are necessary to enhance macrophage activation [4, 7,8,9,10]. This increased activation includes amplified killing mechanisms, such as production of nitric oxide (NO), phagosomal maturation, and increased antigen presentation and co-stimulatory molecule expression [6]. Modulating availability of carbohydrates, lipids, amino acids, and vitamins can have substantial effects on macrophage inflammatory vigor [11,12,13]. A metabolite of particular interest is the amino acid L-arginine
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