Helminth infections drive heterogeneity in human type 2 and regulatory cells
Karin de Ruiter (Leiden University Medical Center)
Simon P. Jochems (Leiden University Medical Center)
Dicky L. Tahapary (Universitas Indonesia, Leiden University Medical Center)
Koen A. Stam (Leiden University Medical Center)
Marion König (Leiden University Medical Center)
Vincent van Unen (Leiden University Medical Center)
Thomas Höllt (Leiden University Medical Center, TU Delft - Computer Graphics and Visualisation)
Moustapha Mbow (Cheikh Anta Diop University of Dakar (UCAD))
Boudewijn P.F. Lelieveldt (Leiden University Medical Center, TU Delft - Pattern Recognition and Bioinformatics)
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Abstract
Helminth infections induce strong type 2 and regulatory responses, but the degree of heterogeneity of such cells is not well characterized. Using mass cytometry, we profiled these cells in Europeans and Indonesians not exposed to helminths and in Indonesians residing in rural areas infected with soil-transmitted helminths. To assign immune alteration to helminth infection, the profiling was performed before and 1 year after deworming. Very distinct signatures were found in Europeans and Indonesians, showing expanded frequencies of T helper 2 cells, particularly CD161+ cells and ILC2s in helminth-infected Indonesians, which was confirmed functionally through analysis of cytokine-producing cells. Besides ILC2s and CD4+ T cells, CD8+ T cells and γδ T cells in Indonesians produced type 2 cytokines. Regulatory T cells were also expanded in Indonesians, but only those expressing CTLA-4, and some coexpressed CD38, HLA-DR, ICOS, or CD161. CD11c+ B cells were found to be the main IL-10 producers among B cells in Indonesians, a subset that was almost absent in Europeans. A number of the distinct immune profiles were driven by helminths as the profiles reverted after clearance of helminth infections. Moreover, Indonesians with no helminth infections residing in an urban area showed immune profiles that resembled Europeans rather than rural Indonesians, which excludes a major role for ethnicity. Detailed insight into the human type 2 and regulatory networks could provide opportunities to target these cells for more precise interventions.
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