Rv3722c governs aspartate-dependent nitrogen metabolism in<i>Mycobacterium tuberculosis</i>

Jansen, Robert S.; Mandyoli, Lungelo; Hughes, Ryan; Wakabayashi, Shoko; Pinkham, Jessica T.; Selbach, Bruna Pelegrim; Guinn, Kristine M.; Rubin, Eric; Sacchettini, James C.; Rhee, Kyu Y.

doi:10.1101/784462

Cited by 3 publications

(3 citation statements)

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“…In contrast, in prokaryotes, including MTB, it is mainly produced from L-aspartate and dihydroxyacetone phosphate by the enzymes encoded by nadA (quinolinic acid synthetase) and nadB (L-aspartate oxidase) (232). Therefore, we propose that a drug to target nadA/B may be an alternative to QPRT inhibitors to control tuberculosis (233).…”

Section: Prospects For Sirtuin Modulators As Drugs Against Tuberculosismentioning

confidence: 96%

Sirtuin-dependent metabolic and epigenetic regulation of macrophages during tuberculosis

et al. 2023

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Macrophages are the preeminent phagocytic cells which control multiple infections. Tuberculosis a leading cause of death in mankind and the causative organism Mycobacterium tuberculosis (MTB) infects and persists in macrophages. Macrophages use reactive oxygen and nitrogen species (ROS/RNS) and autophagy to kill and degrade microbes including MTB. Glucose metabolism regulates the macrophage-mediated antimicrobial mechanisms. Whereas glucose is essential for the growth of cells in immune cells, glucose metabolism and its downsteam metabolic pathways generate key mediators which are essential co-substrates for post-translational modifications of histone proteins, which in turn, epigenetically regulate gene expression. Herein, we describe the role of sirtuins which are NAD+-dependent histone histone/protein deacetylases during the epigenetic regulation of autophagy, the production of ROS/RNS, acetyl-CoA, NAD+, and S-adenosine methionine (SAM), and illustrate the cross-talk between immunometabolism and epigenetics on macrophage activation. We highlight sirtuins as emerging therapeutic targets for modifying immunometabolism to alter macrophage phenotype and antimicrobial function.

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Section: Prospects For Sirtuin Modulators As Drugs Against Tuberculosismentioning

confidence: 96%

Sirtuin-dependent metabolic and epigenetic regulation of macrophages during tuberculosis

et al. 2023

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Section: Prospects For Sirtuin Modulators As Drugs Against Tuberculosismentioning

confidence: 99%

Epigenetic Regulation of Autophagy in Inflammatory Diseases

2024

Frontiers Research Topics

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Frontiers is more than just an open access publisher of scholarly articles: it is a pioneering approach to the world of academia, radically improving the way scholarly research is managed. The grand vision of Frontiers is a world where all people have an equal opportunity to seek, share and generate knowledge. Frontiers provides immediate and permanent online open access to all its publications, but this alone is not enough to realize our grand goals. Frontiers journal seriesThe Frontiers journal series is a multi-tier and interdisciplinary set of openaccess, online journals, promising a paradigm shift from the current review, selection and dissemination processes in academic publishing. All Frontiers journals are driven by researchers for researchers; therefore, they constitute a service to the scholarly community. At the same time, the Frontiers journal series operates on a revolutionary invention, the tiered publishing system, initially addressing specific communities of scholars, and gradually climbing up to broader public understanding, thus serving the interests of the lay society, too. Dedication to qualityEach Frontiers article is a landmark of the highest quality, thanks to genuinely collaborative interactions between authors and review editors, who include some of the world's best academicians. Research must be certified by peers before entering a stream of knowledge that may eventually reach the public -and shape society; therefore, Frontiers only applies the most rigorous and unbiased reviews. Frontiers revolutionizes research publishing by freely delivering the most outstanding research, evaluated with no bias from both the academic and social point of view. By applying the most advanced information technologies, Frontiers is catapulting scholarly publishing into a new generation. What are Frontiers Research Topics?Frontiers Research Topics are very popular trademarks of the Frontiers journals series: they are collections of at least ten articles, all centered on a particular subject. With their unique mix of varied contributions from Original Research to Review Articles, Frontiers Research Topics unify the most influential researchers, the latest key findings and historical advances in a hot research area.

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“…Nitrogen from aspartate is assimilated into various amino acids and is used to synthesize biomass. Rv3722, a recently assigned aspartate aminotransferase that Downloaded from http://portlandpress.com/bioscirep/article-pdf/doi/10.1042/BSR20211215/928211/bsr-2021-1215c.pdf by guest on 31 January 2022 facilitated aspartate-dependent nitrogen transfer to form glutamate from 2-oxoglutarate was important for in vitro growth and for virulence in mice and macrophages (74). Asparaginase, ansA is essential to assimilate nitrogen from asparagine and to resist acid stress in the phagosomes (75).…”

Section: Nitrogen Metabolic Fluxesmentioning

confidence: 99%

Mycobacterium tuberculosis carbon and nitrogen metabolic fluxes

Pooja

Borah

2022

Bioscience Reports

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Mycobacterium tuberculosis (Mtb) is one of the most formidable pathogens causing tuberculosis (TB), a devastating infectious disease responsible for the highest human mortality and morbidity. The emergence of drug resistant strains of the pathogen has increased the burden of TB tremendously and new therapeutics to overcome the problem of drug resistance are urgently needed. Metabolism of Mtb and its interactions with the host is important for its survival and virulence; this is an important topic of research where there is growing interest in developing new therapies and drugs that target these interactions and metabolism of the pathogen during infection. Mtb adapts its metabolism in its intracellular niche and acquires multiple nutrient sources from the host cell. Carbon metabolic pathways and fluxes of Mtb has been extensively researched for over a decade and is well-defined. Recently, there has been investigations and efforts to measure metabolism of nitrogen, which is another important nutrient for Mtb during infection. This review discusses our current understanding of the central carbon and nitrogen metabolism, and metabolic fluxes that are important for the survival of the TB pathogen.

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Rv3722c governs aspartate-dependent nitrogen metabolism inMycobacterium tuberculosis

Cited by 3 publications

References 75 publications

Sirtuin-dependent metabolic and epigenetic regulation of macrophages during tuberculosis

Sirtuin-dependent metabolic and epigenetic regulation of macrophages during tuberculosis

Epigenetic Regulation of Autophagy in Inflammatory Diseases

Mycobacterium tuberculosis carbon and nitrogen metabolic fluxes

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