Tomi Mori scite author profile

Rationale: The immunologic events surrounding primary Mycobacterium tuberculosis infection and development of tuberculosis remain controversial. Young children who develop tuberculosis do so quickly after first exposure, thus permitting study of immune response to primary infection and disease. We hypothesized that M. tuberculosis-specific CD8 1 T cells are generated in response to high bacillary loads occurring during tuberculosis. Objectives: To determine if M. tuberculosis-specific T cells are generated among healthy children exposed to M. tuberculosis and children with tuberculosis.Methods: Enzyme-linked immunosorbent spot assays were used to measure IFN-g production in response to M. tuberculosis-specific proteins ESAT-6/CFP-10 by peripheral blood mononuclear cells and CD8 1 T cells isolated from Ugandan children hospitalized with tuberculosis (n ¼ 96) or healthy tuberculosis contacts (n ¼ 62). Measurements and Main Results: The proportion of positive CD8 1 T-cell assays and magnitude of CD81 T-cell responses were significantly greater among young (,5 yr) tuberculosis cases compared with young contacts (P ¼ 0.02, Fisher exact test, P ¼ 0.01, Wilcoxon rank-sum, respectively). M. tuberculosis-specific T-cell responses measured in peripheral blood mononuclear cells were equivalent between groups. Conclusions: Among young children, M. tuberculosis-specific CD8 1 T cells develop in response to high bacillary loads, as occurs during tuberculosis, and are unlikely to be found after M. tuberculosis exposure. T-cell responses measured in peripheral blood mononuclear cells are generated after M. tuberculosis exposure alone, and thus cannot distinguish exposure from disease. In young children, IFN-g-producing M. tuberculosis-specific CD8 1 T cells provide an immunologic signature of primary M. tuberculosis infection resulting in disease.

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Comprehensive definition of human immunodominant CD8 antigens in tuberculosis

Lewinsohn

Swarbrick

Park

et al. 2017

npj Vaccines

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Despite widespread use of the Bacillus Calmette-Guerin vaccine, tuberculosis, caused by infection with Mycobacterium tuberculosis, remains a leading cause of morbidity and mortality worldwide. As CD8+ T cells are critical to tuberculosis host defense and a phase 2b vaccine trial of modified vaccinia Ankara expressing Ag85a that failed to demonstrate efficacy, also failed to induce a CD8+ T cell response, an effective tuberculosis vaccine may need to induce CD8+ T cells. However, little is known about CD8, as compared to CD4, antigens in tuberculosis. Herein, we report the results of the first ever HLA allele independent genome-wide CD8 antigen discovery program. Using CD8+ T cells derived from humans with latent tuberculosis infection or tuberculosis and an interferon-γ ELISPOT assay, we screened a synthetic peptide library representing 10% of the Mycobacterium tuberculosis proteome, selected to be enriched for Mycobacterium tuberculosis antigens. We defined a set of immunodominant CD8 antigens including part or all of 74 Mycobacterium tuberculosis proteins, only 16 of which are previously known CD8 antigens. Immunogenicity was associated with the degree of expression of mRNA and protein. Immunodominant antigens were enriched in cell wall proteins with preferential recognition of Esx protein family members, and within proteins comprising the Mycobacterium tuberculosis secretome. A validation study of immunodominant antigens demonstrated that these antigens were strongly recognized in Mycobacterium tuberculosis-infected individuals from a tuberculosis endemic region in Africa. The tuberculosis vaccine field will likely benefit from this greatly increased known repertoire of CD8 immunodominant antigens and definition of properties of Mycobacterium tuberculosis proteins important for CD8 antigenicity.

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The Pandemic Experience: A Corpus of Subjective Reports on Life During the First Wave of COVID-19 in the UK, Japan, and Mexico

Froese

Broome

Carel

et al. 2021

Front. Public Health

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Tomi Mori

Effect of Mode of Delivery on the Incidence of Urinary Incontinence in Primiparous Women

Patient Activation and Improved Outcomes in HIV-Infected Patients

CD8⁺T Cells Provide an Immunologic Signature of Tuberculosis in Young Children

Comprehensive definition of human immunodominant CD8 antigens in tuberculosis

The Pandemic Experience: A Corpus of Subjective Reports on Life During the First Wave of COVID-19 in the UK, Japan, and Mexico

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Tomi Mori

Effect of Mode of Delivery on the Incidence of Urinary Incontinence in Primiparous Women

Patient Activation and Improved Outcomes in HIV-Infected Patients

CD8+T Cells Provide an Immunologic Signature of Tuberculosis in Young Children

Comprehensive definition of human immunodominant CD8 antigens in tuberculosis

The Pandemic Experience: A Corpus of Subjective Reports on Life During the First Wave of COVID-19 in the UK, Japan, and Mexico

Contact Info

Product

Resources

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CD8⁺T Cells Provide an Immunologic Signature of Tuberculosis in Young Children