Eukaryotic-like Adenylyl Cyclases in Mycobacterium tuberculosis H37Rv

Reddy, Sathyavelu K.; Kamireddi, Madhavi; Dhanireddy, Kiran; Young, Lynn; Davis, A. W.; Reddy, P.G.

doi:10.1074/jbc.m104108200

Cited by 54 publications

(63 citation statements)

References 32 publications

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“…One caveat here is that although the main effects are likely to be due to activity of macrophage enzymes we cannot rule out the fact that the effectors and/or inhibitors we used may also target the equivalent enzymes known to be expressed by the mycobacteria themselves (Shenoy et al, 2005;Lowrie et al, 1975;Castro et al, 2005;Cann et al, 2003;Reddy et al, 2001). Complex effects of modulating cAMP levels in mycobacterium-infected macrophages have been described in many studies making it difficult to provide a simple model (e.g.…”

Section: Discussionmentioning

confidence: 99%

“…This system mediates a plethora of cellular functions with extensive 'cross-talk' occurs between it and other signaling networks throughout cells (Beavo and Brunton, 2002;Antoni, 2000;Ellerbroek et al, 2003;Frisch, 2000;Houslay and Kolch, 2000;Tasken and Anandahl, 2004;Wong and Scott, 2004;Houslay, 1998;Housley and Milligan, 1997;Howe and Juliano, 2000). Increases in cAMP levels generally compromise the bactericidal activity of the host immune system (Bengis-Garber and Gruener, 1996;Gueirard et al, 1998;Khelef et al, 1993;Reddy et al, 2001). Many pathogens have taken advantage of this phenomenon and evolved mechanisms to elevate intracellular cAMP levels in both macrophages (Gross et al, 2003;Hanski, 1989) and neutrophils (Confer and Eaton, 1982;Gross et al, 2003;Hanski, 1989;Nathan, 2003) -evidently to facilitate their survival within phagosomes.…”

Section: Introductionmentioning

confidence: 99%

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cAMP synthesis and degradation by phagosomes regulate actin assembly and fusion events: consequences for mycobacteria

Kalamidas

Kuehnel

Peyron

et al. 2006

Journal of Cell Science

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We showed recently that actin assembly by phagosomal membranes facilitates fusion with late endocytic organelles in macrophages. Moreover, lipids that induced phagosomal actin also stimulated this fusion process. In macrophages infected with pathogenic mycobacteria actin-stimulatory lipids led to an increase in pathogen destruction, whereas inhibitors facilitated their growth. A model was proposed whereby phagosomal membrane actin assembly provides tracks for lysosomes to move towards phagosomes, thereby facilitating fusion. Here, we investigated how cAMP affected phagosomal actin assembly in vitro, and phagosomal actin, acidification and late fusion events in J774 macrophages. Latex bead phagosomes are shown to possess adenylyl cyclase activity, which synthesizes cAMP, and phosphodiesterase activity, which degrades cAMP. The system is regulated by protein kinase A (PKA). Increasing cAMP levels inhibited, whereas decreasing cAMP levels stimulated, actin assembly in vitro and within cells. Increasing cAMP levels also inhibited phagosome-lysosome fusion and acidification in cells, whereas reducing cAMP had the opposite effect. High cAMP levels induced an increase in intraphagosomal growth in macrophages of both the non-pathogenic Mycobacterium smegmatis and the pathogenic Mycobacterium tuberculosis, whereas low cAMP levels or inhibition of PKA correlated with increased bacterial destruction. We argue that the phagosome cAMP-PKA system behaves as a molecular switch that regulates phagosome actin and maturation in macrophages.

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Section: Discussionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

cAMP synthesis and degradation by phagosomes regulate actin assembly and fusion events: consequences for mycobacteria

Kalamidas

Kuehnel

Peyron

et al. 2006

Journal of Cell Science

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“…All candidate open reading frames contained a cyclase homology domain associated with one of a variety of cytoplasmic, receptor-type, and integral membrane structural motifs (35). Two of these genes (Rv1625c and Rv2435c) belong to the mammalian type adenylyl cyclase grouping, and both enzymes are active (19,28,35,50,54). Functionality has also been shown for the mycobacterial cyclases Rv1264, Rv1318c, Rv1319c, Rv1320c, and Rv3645 (6,27).…”

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confidence: 99%

Identification of Cyclic AMP-Regulated Genes in Mycobacterium tuberculosis Complex Bacteria under Low-Oxygen Conditions

Gazdik

McDonough

2005

J Bacteriol

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Mycobacterium tuberculosis is the etiological agent of tuberculosis (TB), which kills approximately 2 million people a year despite current treatment options. A greater understanding of the biology of this bacterium is needed to better combat TB disease. The M. tuberculosis genome encodes as many as 15 adenylate cyclases, suggesting that cyclic AMP (cAMP) has an important, yet overlooked, role in mycobacteria. This study examined the effect of exogenous cAMP on protein expression in Mycobacterium bovis BCG grown under hypoxic versus ambient conditions. Both shaking and shallow standing cultures were examined for each atmospheric condition. Different cAMP-dependent changes in protein expression were observed in each condition by two-dimensional gel electrophoresis. Shaking low-oxygen cultures produced the most changes (12), while standing ambient conditions showed the fewest (2). Five upregulated proteins, Rv1265, Rv2971, GroEL2, PE_PGRS6a, and malate dehydrogenase, were identified from BCG by mass spectrometry and were shown to also be regulated by cAMP at the mRNA level in both M. tuberculosis H37Rv and BCG. To our knowledge, these data provide the first direct evidence for cAMP-mediated gene regulation in TB complex mycobacteria.Tuberculosis (TB) is a leading cause of human death by an infectious agent, killing approximately 2 million people each year. Nearly one-third of the world's population is latently infected with the Mycobacterium tuberculosis bacillus, and 7 to 8 million new TB cases occur annually (49). A deadly synergy with the human immunodeficiency virus epidemic and an increasing proportion of drug-resistant cases contribute to TB's recent resurgence and complicate its treatment (7, 9). A better understanding of M. tuberculosis biology is needed to devise more effective treatments against TB. Gene regulation is critical for the interaction of the tubercle bacilli with their

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“…We expressed amino acids 160 to 353 of cyaB as a recombinant protein (cyaB ) that contained a threonine residue (T293) at the position corresponding to cyaB1 T721 ( Figure 1A). cyaB 160 Mycobacterium tuberculosis H37Rv is a gram-negative bacterium and important human pathogen for which the genome has revealed a number of putative class III ACs (15,21,22). We expressed two ACs that contain either a threonine (amino acids 356-535 of Rv1319c) or an aspartate (Rv1264 holoenzyme) at the position corresponding to T721 of cyaB1 ( Figure 1A).…”

Section: Ac Assaymentioning

confidence: 99%