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Prostaglandins differentially modulate mucosal‐associated invariant T‐cell activation and function according to stimulus

Mucosal‐associated invariant T (MAIT) cells are an innate‐like T‐cell type conserved in many mammals and especially abundant in humans. Their semi‐invariant T‐cell receptor (TCR) recognizes the major histocompatibility complex–like molecule… Click to show full abstract

Mucosal‐associated invariant T (MAIT) cells are an innate‐like T‐cell type conserved in many mammals and especially abundant in humans. Their semi‐invariant T‐cell receptor (TCR) recognizes the major histocompatibility complex–like molecule MR1 presenting riboflavin intermediates associated with microbial metabolism. Full MAIT cell triggering requires costimulation via cytokines, and the cells can also be effectively triggered in a TCR‐independent manner by cytokines [e.g. interleukin (IL)‐12 and IL‐18 in combination]. Thus, triggering of MAIT cells is highly sensitive to local soluble mediators. Suppression of MAIT cell activation has not been well explored and could be very relevant to their roles in infection, inflammation and cancer. Prostaglandins (PG) are major local mediators of these microenvironments which can have regulatory roles for T cells. Here, we explored whether prostaglandins suppressed MAIT cell activation in response to TCR‐dependent and TCR‐independent signals. We found that protaglandin E2 (PGE2) and to a lesser extent protaglandin D2 (PGD2), but not leukotrienes, suppressed MAIT cell responses to Escherichia coli or TCR triggers. However, there was no impact on cytokine‐induced triggering. The inhibition was blocked by targeting the signaling mediated via PG receptor 2 (PTGER2) and 4 (PTGER4) receptors in combination. These data indicate that prostaglandins can potentially modulate local MAIT cell functions in vivo and indicate distinct regulation of the TCR‐dependent and TCR‐independent pathways of MAIT cell activation.

Keywords: cell; tcr; mait; cell activation; mait cell

Journal Title: Immunology and Cell Biology
Year Published: 2022

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