T Regulatory Cells and Immune Activation in <i>Mycobacterium tuberculosis</i> Infection and the Effect of Preventive Therapy

Wergeland, Ida; Aßmus, Jörg; Dyrhol-Riise, Anne Margarita

doi:10.1111/j.1365-3083.2010.02496.x

Cited by 51 publications

(51 citation statements)

References 25 publications

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“…A significant correlation was not observed for persons with latent M. tuberculosis infection. Our findings differ from a previous study that recently found a positive correlation between Treg cell frequency and the frequency of CD4 ϩ CD38 ϩ HLA-DR ϩ T cells in healthy uninfected controls but not among subjects with active tuberculosis disease or latent M. tuberculosis infection (54). One reason that we may have observed different results could be because we compared immune activation between persons with pulmonary and extrapulmonary tuberculosis, whereas the referenced study combined these two patient groups.…”

Section: Discussioncontrasting

confidence: 55%

“…The perturbation of the immunologic environment during M. tuberculosis infection is felt to contribute to HIV disease severity and progression in coinfected persons (20). Previous studies have reported increased activation of CD4 ϩ and CD8 ϩ T lymphocytes in active tuberculosis and latent infection (4,24,43,44,54). These studies have either studied only persons with pulmonary tuberculosis or evaluated pulmonary and extrapulmonary tuberculosis together as one entity.…”

Section: Discussionmentioning

confidence: 99%

See 1 more Smart Citation

Increased Frequency of Regulatory T Cells and T Lymphocyte Activation in Persons with Previously Treated Extrapulmonary Tuberculosis

Almeida

Fiske

Sterling

et al. 2012

Clin Vaccine Immunol

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Section: Discussioncontrasting

confidence: 55%

Section: Discussionmentioning

confidence: 99%

Increased Frequency of Regulatory T Cells and T Lymphocyte Activation in Persons with Previously Treated Extrapulmonary Tuberculosis

Almeida

Fiske

Sterling

et al. 2012

Clin Vaccine Immunol

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“…While individuals with latent or asymptomatic infection exhibit normal or slightly elevated Treg numbers in their blood [60, 61], those with active TB tend to show increased numbers of Tregs in the blood and at sites of infection (lung and pleural sac) [62-65]. Histological analysis has further shown that cavitating granulomas, those that generally possess the highest bacterial burden, contain significantly more Tregs than other types of granulomas [66].…”

Section: Regulation Of Adaptive Immunity Against Mtbmentioning

confidence: 99%

Understanding and overcoming the barriers to T cell-mediated immunity against tuberculosis

Urdahl

2014

Seminars in Immunology

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Despite the overwhelming success of immunization in reducing, and even eliminating, the global threats posed by a wide spectrum of infectious diseases, attempts to do the same for tuberculosis (TB) have failed to date. While most effective vaccines act by eliciting neutralizing antibodies, T cells are the primary mediators of adaptive immunity against TB. Unfortunately, the onset of the T cell response after aerosol infection with Mycobacterium tuberculosis (Mtb), the bacterium that causes TB, is exceedingly slow, and systemically administered vaccines only modestly accelerate the recruitment of effector T cells to the lungs. This delay seems to be orchestrated by Mtb itself to prolong the period of unrestricted bacterial replication in the lung that characterizes the innate phase of the response. When T cells finally arrive at the site of infection, multiple layers of regulation have been established that limit the ability of T cells to control or eradicate Mtb. From this understanding, emerges a strategy for achieving immunity. Lung resident memory T cells may recognize Mtb-infected cells shortly after infection and confer protection before regulatory networks are allowed to develop. Early studies using vaccines that elicit lung resident T cells by targeting the lung mucosa have been promising, but many questions remain. Due to the fundamental nature of these questions, and the need to understand and manipulate the early events in the lung after aerosol infection, only coordinated approaches that utilize tractable animal models to inform human TB vaccine trials will move the field towards its goal.

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“…Highly differentiated circulating effector T cells have a limited lifespan (i.e., months) (24) and disappear or greatly decrease after removal of antigen after bacterial clearance and cessation of antigen presentation (i.e., completion of LTBI treatment) (25). Several prior studies have described activated effector T-cell phenotypes in active TB and LTBI in animal models and ex vivo human studies (4,(26)(27)(28)(29)(30)(31)(32). Moreover, antibiotic treatment is known to alter the phenotype and transcriptome of circulating T-lymphocytes in patients with active TB infection, although little is known of the effects after LTBI treatment (31,33).…”

Section: Original Articlementioning

confidence: 99%

Combinatorial Immunoprofiling in Latent Tuberculosis Infection. Toward Better Risk Stratification

Escalante

Peikert

Keulen³

et al. 2015

Am J Respir Crit Care Med

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Rationale: Most immunocompetent patients diagnosed with latent tuberculosis infection (LTBI) will not progress to tuberculosis (TB) reactivation. However, current diagnostic tools cannot reliably distinguish nonprogressing from progressing patients a priori, and thus LTBI therapy must be prescribed with suboptimal patient specificity. We hypothesized that LTBI diagnostics could be improved by generating immunomarker profiles capable of categorizing distinct patient subsets by a combinatorial immunoassay approach.Objectives: A combinatorial immunoassay analysis was applied to identify potential immunomarker combinations that distinguish among unexposed subjects, untreated patients with LTBI, and treated patients with LTBI and to differentiate risk of reactivation.Methods: IFN-g release assay (IGRA) was combined with a flow cytometric assay that detects induction of CD25 1 CD134 1 coexpression on TB antigen-stimulated T cells from peripheral blood. The combinatorial immunoassay analysis was based on receiver operating characteristic curves, technical cut-offs, 95% bivariate normal density ellipse prediction, and statistical analysis. Risk of reactivation was estimated with a prediction formula.Measurements and Main Results: Sixty-five out of 150 subjects were included. The combinatorial immunoassay approach identified at least four different T-cell subsets. The representation of these immune phenotypes was more heterogeneous in untreated patients with LTBI than in treated patients with LTBI or unexposed groups. Patients with IGRA(1) CD41 CD25 1 CD134 1 T-cell phenotypes had the highest estimated reactivation risk (4.11 6 2.11%).Conclusions: These findings suggest that immune phenotypes defined by combinatorial assays may potentially have a role in identifying those at risk of developing TB; this potential role is supported by risk of reactivation modeling. Prospective studies will be needed to test this novel approach.

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T Regulatory Cells and Immune Activation in Mycobacterium tuberculosis Infection and the Effect of Preventive Therapy

Cited by 51 publications

References 25 publications

Increased Frequency of Regulatory T Cells and T Lymphocyte Activation in Persons with Previously Treated Extrapulmonary Tuberculosis

Increased Frequency of Regulatory T Cells and T Lymphocyte Activation in Persons with Previously Treated Extrapulmonary Tuberculosis

Understanding and overcoming the barriers to T cell-mediated immunity against tuberculosis

Combinatorial Immunoprofiling in Latent Tuberculosis Infection. Toward Better Risk Stratification

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