Extracellular Vesicles from Candidozyma (Candida) auris inhibit proliferation of CD4 T cells by disrupting the IL-2 Axis

Candidozyma auris (formerly Candida auris) is an emerging multidrug-resistant pathogenic fungus that has rapidly spread across the world. Due to the high frequency of multidrug resistant strains and mortality rate, C. auris is considered a critical health threat by the CDC and the WHO. Like other pathogens, C. auris employs virulence factors that are delivered by extracellular vesicles (EVs). We have shown that EVs from C. auris (CauEVs) activate murine phagocytes, boosting innate immune mechanisms. However, the effect of fungal EVs on lymphoid cells has not yet been addressed. Upon activation, CD4 T cells undergo clonal expansion and cytokine production that orchestrate immune responses to eradicate invading pathogens, a process of critical importance in controlling invasive candidiasis. Here we show that the treatment with CauEVs inhibited the activation-induced CD4 T cells proliferation in a dose-dependent manner. Notably, we found that CauEVs acted at early events downstream to the TCR signaling, inhibiting the MAP kinase phosphorylation. Interestingly, the inhibition of CD4 T cell proliferation by CauEVs was associated with a dramatic increase on the IL-2 production, while blocking the IL-2 downstream signaling. Taken together, our results suggest that CauEVs may contain an immunomodulatory factor(s) that affect the CD4 T cell activation and their fate from early to later events in a previously undescribed mechanism.