Hypervirulent mutant of<i>Mycobacterium tuberculosis</i>resulting from disruption of the<i>mce1</i>operon

Shimono, Nobuyuki; Morici, Lisa A.; Coppola, Nicola; Cantrell, Sally A.; Sidders, Ben; Ehrt, Sabine; Riley, Lee W.

doi:10.1073/pnas.2433882100

Cited by 204 publications

(238 citation statements)

References 22 publications

(28 reference statements)

Supporting

Mentioning

216

Contrasting

Unclassified

Order By: Relevance

“…Previous studies have implicated the mce operon (53) and several two-component signaling modules (54) as additional negative regulators of M. tuberculosis virulence. In these studies, however, the pleiotropic nature of the mutants may complicate efforts to define the molecular underpinnings of the phenotype.…”

Section: Discussionmentioning

confidence: 99%

A sulfated metabolite produced bystf3negatively regulates the virulence ofMycobacteriumtuberculosis

Mougous

Senaratne

Kim

et al. 2006

Proc. Natl. Acad. Sci. U.S.A.

Self Cite

View full text Add to dashboard Cite

Sulfated molecules have been shown to modulate isotypic interactions between cells of metazoans and heterotypic interactions between bacterial pathogens or symbionts and their eukaryotic host cells. Mycobacterium tuberculosis, the causative agent of tuberculosis, produces sulfated molecules that have eluded functional characterization for decades. We demonstrate here that a previously uncharacterized sulfated molecule, termed S881, is localized to the outer envelope of M. tuberculosis and negatively regulates the virulence of the organism in two mouse infection models. Furthermore, we show that the biosynthesis of S881 relies on the universal sulfate donor 3 -phosphoadenosine-5 -phosphosulfate and a previously uncharacterized sulfotransferase, stf3. These findings extend the known functions of sulfated molecules as general modulators of cell-cell interactions to include those between a bacterium and a human host.Fourier transform ion cyclotron resonance ͉ hypervirulent ͉ sulfate assimilation ͉ kinase ͉ adenosine-5-phosphosulfate A wide variety of organisms use sulfated molecules to control extracellular events. In mammals, sulfation of tyrosine residues on cell surface proteins is important for the interactions of chemokines with certain chemokine receptors, and for viral binding and entry (1-6). Sulfated glycans modulate processes such as leukocyte homing to lymph nodes, clearance of serum glycoproteins, and blood coagulation (7-9). Members of the glypican family that are modified with sulfated glycosaminoglycans guide organ development in Drosophila by maintaining a morphogen concentration gradient (10).In bacteria, sulfated glycolipids have been shown to serve as extracellular signaling molecules (11). The nitrogen fixing bacterium Sinorhizobium meliloti secretes the nodulation factor NodRm-1, a tetrasaccharide bearing both sulfate and lipid modifications (12). This molecule binds a receptor on the host plant, normally alfalfa, and induces root nodule formation. The sulfate group is critical for the function of NodRm-1, because the unsulfated form fails to induce root nodulation in alfalfa. In the rice blight-causing pathogen Xanthomonas oryzae, several genes involved in the synthesis of sulfated metabolites have been identified as avirulence factors with respect to certain host strains (13,14). These examples suggest that bacterial sulfated metabolites can participate in dialogue with eukaryotic hosts, analogous to their role in mammalian cell-cell communication.Mycobacteria produce an unusually complex array of sulfated structures (11). Sulfolipid-1 (SL-1), an abundant component of the cell envelope of M. tuberculosis, is the best characterized of these molecules. SL-1 has generated much interest because of its elaborate structure and the observation that its abundance correlates with strain virulence (15)(16)(17)(18)(19)(20)(21)(22). Advances in M. tuberculosis genetics and genome sequence data facilitated several contemporary studies that addressed aspects of the biosynthesis and the function of SL-1 in v...

show abstract

Section: Discussionmentioning

confidence: 99%

A sulfated metabolite produced bystf3negatively regulates the virulence ofMycobacteriumtuberculosis

Mougous

Senaratne

Kim

et al. 2006

Proc. Natl. Acad. Sci. U.S.A.

Self Cite

View full text Add to dashboard Cite

show abstract

“…Both groups suggested that the operon might encode an importer system involved in recycling of MA. Also, disruption of the mce1operon renders the cells hypervirulent in mice 40,41 . The mutant is unable to induce a strong T-helper 1 (Th1) type T cell immune response and organized granuloma formation in lungs 41 .…”

Section: Mycolic Acidsmentioning

confidence: 99%

Bacterial immunostat: Mycobacterium tuberculosis lipids and their role in the host immune response

Queiroz

Riley

2017

Rev. Soc. Bras. Med. Trop.

Self Cite

View full text Add to dashboard Cite

The lipid-rich cell wall of Mycobacterium tuberculosis is a dynamic structure that is involved in the regulation of the transport of nutrients, toxic host-cell effector molecules, and anti-tuberculosis drugs. It is therefore postulated to contribute to the longterm bacterial survival in an infected human host. Accumulating evidence suggests that M. tuberculosis remodels the lipid composition of the cell wall as an adaptive mechanism against host-imposed stress. Some of these lipid species (trehalose dimycolate, diacylated sulphoglycolipid, and mannan-based lipoglycans) trigger an immunopathologic response, whereas others (phthiocerol dimycocerosate, mycolic acids, sulpholipid-1, and di-and polyacyltrehalose) appear to dampen the immune responses. These lipids appear to be coordinately expressed in the cell wall of M. tuberculosis during different phases of infection, ultimately determining the clinical fate of the infection. This review summarizes the current state of knowledge on the metabolism, transport, and homeostatic or immunostatic regulation of the cell wall lipids, and their orchestrated interaction with host immune responses that results in bacterial clearance, persistence, or tuberculosis.

show abstract

“…Thus interaction with epithelia is thought to be crucial for dissemination and to dominate the disease outcome. Besides HBHA, M. tuberculosis has another possible adhesin, designated mycobacterial cell entry protein 1 (Mcep1), of which DNA fragmentation confers on Escherichia coli an ability to invade into nonphagocytic HeLa cells (9), although its precise role as an adhesin remains unclear (10). It is likely that myco-bacteria utilize multiple adhesins to promote attachment to nonprofessional phagocytes.…”

mentioning

confidence: 99%

Extracellular Mycobacterial DNA-binding Protein 1 Participates in Mycobacterium-Lung Epithelial Cell Interaction through Hyaluronic Acid

Aoki

Matsumoto

Hirayama

et al. 2004

Journal of Biological Chemistry

View full text Add to dashboard Cite

Hypervirulent mutant ofMycobacterium tuberculosisresulting from disruption of themce1operon

Cited by 204 publications

References 22 publications

A sulfated metabolite produced bystf3negatively regulates the virulence ofMycobacteriumtuberculosis

A sulfated metabolite produced bystf3negatively regulates the virulence ofMycobacteriumtuberculosis

Bacterial immunostat: Mycobacterium tuberculosis lipids and their role in the host immune response

Extracellular Mycobacterial DNA-binding Protein 1 Participates in Mycobacterium-Lung Epithelial Cell Interaction through Hyaluronic Acid

Contact Info

Product

Resources

About