Peripheral Blood Mucosal-Associated Invariant T Cells in Tuberculosis Patients and Healthy Mycobacterium tuberculosis-Exposed Controls

Suliman, Sara; Gela, Anele; Mendelsohn, Simon C.; Iwany, Sarah K.; Tamara, Kattya Lopez; Mabwe, Simbarashe; Bilek, Nicole; Darboe, Fatoumatta; Fisher, Michelle; Corbett, Alexandra J.; Kjer‐Nielsen, Lars; Eckle, Sidonia B G; Huang, Chuan; Zhang, Zibiao; Lewinsohn, David; McCluskey, James; Rossjohn, Jamie; Hatherill, Mark; León, Segundo R.; Calderón, Róger; Lecca, Leonid; Murray, Megan; Scriba, Thomas J.; Rhijn, Ildiko Van; Moody, D. Branch

doi:10.1093/infdis/jiaa173

Cited by 21 publications

(28 citation statements)

References 51 publications

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“…Wong et al (17) found a trend toward decreased frequency of CD161 hi CD8 + T cells in PBMCs from LTBI compared with controls in a TB-endemic African setting. Other studies have found no difference in MAIT frequencies in LTBI compared with TB neg, or even an increase (16,18). These contradictory results may be explained by variations in M. tuberculosis exposure rates in endemic versus nonendemic TB areas, how well the latent infection is controlled, as well as a difference in how MAIT populations were defined.…”

Section: Discussionmentioning

confidence: 88%

“…One of the most frequent nonclassically restricted T cell populations in the blood are MR1-restricted T cells, which decrease in frequency in active TB (14,15). For LTBI, there have been contradicting results regarding the frequency of MAITs in PBMCs (14,(16)(17)(18). MR1-restricted T cells represent a significant fraction of CD8 + and CD4 -CD8 -T cells in peripheral blood (19,20).…”

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confidence: 99%

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Quantitative and Qualitative Perturbations of CD8+ MAITs in Healthy Mycobacterium tuberculosis–Infected Individuals

et al. 2020

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CD8 T cells are considered important contributors to the immune response against Mycobacterium tuberculosis, yet limited information is currently known regarding their specific immune signature and phenotype. In this study, we applied a cell population transcriptomics strategy to define immune signatures of human latent tuberculosis infection (LTBI) in memory CD8 T cells. We found a 41-gene signature that discriminates between memory CD8 T cells from healthy LTBI subjects and uninfected controls. The gene signature was dominated by genes associated with mucosal-associated invariant T cells (MAITs) and reflected the lower frequency of MAITs observed in individuals with LTBI. There was no evidence for a conventional CD8 T cell-specific signature between the two cohorts. We, therefore, investigated MAITs in more detail based on Va7.2 and CD161 expression and staining with an MHC-related protein 1 (MR1) tetramer. This revealed two distinct populations of CD8 + Va7.2 + CD161 + MAITs: MR1 tetramer + and MR1 tetramer 2 , which both had distinct gene expression compared with memory CD8 T cells. Transcriptomic analysis of LTBI versus noninfected individuals did not reveal significant differences for MR1 tetramer + MAITs. However, gene expression of MR1 tetramer 2 MAITs showed large interindividual diversity and a tuberculosis-specific signature. This was further strengthened by a more diverse TCR-a and-b repertoire of MR1 tetramer 2 cells as compared with MR1 tetramer +. Thus, circulating memory CD8 T cells in subjects with latent tuberculosis have a reduced number of conventional MR1 tetramer + MAITs as well as a difference in phenotype in the rare population of MR1 tetramer 2 MAITs compared with uninfected controls. ImmunoHorizons, 2020, 4: 292-307.

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Section: Discussionmentioning

confidence: 88%

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confidence: 99%

Quantitative and Qualitative Perturbations of CD8+ MAITs in Healthy Mycobacterium tuberculosis–Infected Individuals

et al. 2020

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“…Next, we wanted to measure the frequency of DAT 2 -reactive T cells in a cohort of 150 human subjects 27 , 28 to determine if there is an Mtb infection or disease-associated expansion of DAT-specific T cells. PBMCs were isolated from 50 Peruvian individuals with active tuberculosis (TB) before the start of anti-TB drug treatment.…”

Section: Resultsmentioning

confidence: 99%

Synthetic mycobacterial diacyl trehaloses reveal differential recognition by human T cell receptors and the C-type lectin Mincle

Reijneveld

Holzheimer

Young

et al. 2021

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The cell wall of Mycobacterium tuberculosis is composed of diverse glycolipids which potentially interact with the human immune system. To overcome difficulties in obtaining pure compounds from bacterial extracts, we recently synthesized three forms of mycobacterial diacyltrehalose (DAT) that differ in their fatty acid composition, DAT1, DAT2, and DAT3. To study the potential recognition of DATs by human T cells, we treated the lipid-binding antigen presenting molecule CD1b with synthetic DATs and looked for T cells that bound the complex. DAT1- and DAT2-treated CD1b tetramers were recognized by T cells, but DAT3-treated CD1b tetramers were not. A T cell line derived using CD1b-DAT2 tetramers showed that there is no cross-reactivity between DATs in an IFN-γ release assay, suggesting that the chemical structure of the fatty acid at the 3-position determines recognition by T cells. In contrast with the lack of recognition of DAT3 by human T cells, DAT3, but not DAT1 or DAT2, activates Mincle. Thus, we show that the mycobacterial lipid DAT can be both an antigen for T cells and an agonist for the innate Mincle receptor, and that small chemical differences determine recognition by different parts of the immune system.

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“…MAIT cells are multifaceted in their functional response to infections and in maintaining homeostasis, also contributing to tissue repair and wound healing 3 . In the context of M. tb , human blood MAIT cell frequencies are reportedly reduced during active infection, 4 suggestive of circulating MAIT cell migration into the tissues, although a recent large cohort study disputes this finding 5 . Human MAIT cells also secrete interferon‐gamma when cultured with M. tb ‐infected antigen‐presenting cells 4 .…”

Section: Figurementioning

confidence: 99%

“…3 In the context of M. tb, human blood MAIT cell frequencies are reportedly reduced during active infection, 4 suggestive of circulating MAIT cell migration into the tissues, although a recent large cohort study disputes this finding. 5 Human MAIT cells also secrete interferon-gamma when cultured with M. tb-infected antigen-presenting cells. 4 Similarly, in mice, MAIT T-cell receptor transgenic cells secrete interferongamma in response to BCG and can inhibit its intracellular growth.…”

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confidence: 99%

When it’s good to have MAITs

2020

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Peripheral Blood Mucosal-Associated Invariant T Cells in Tuberculosis Patients and Healthy Mycobacterium tuberculosis-Exposed Controls

Cited by 21 publications

References 51 publications

Quantitative and Qualitative Perturbations of CD8+ MAITs in Healthy Mycobacterium tuberculosis–Infected Individuals

Quantitative and Qualitative Perturbations of CD8+ MAITs in Healthy Mycobacterium tuberculosis–Infected Individuals

Synthetic mycobacterial diacyl trehaloses reveal differential recognition by human T cell receptors and the C-type lectin Mincle

When it’s good to have MAITs

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