Background: Autosomal Dominant-Hyper-IgE Syndrome (AD-HIES) is caused by dominant-negative (DN) STAT3 mutations and characterized by high IgE levels, a lack of Th17-cells, and recurrent infections with extracellular pathogens. We previously identified an enigmatic population of IL-10 producing CCR6+B-helper T-cells and investigated here their relationship to Th17-cells and STAT3 signaling requirements. Methods: Human blood lymphocytes were analyzed by multiparametric flow cytometry in healthy donors and AD-HIES patients. Analysis was performed by conventional gating or with bioinformatic tools. FACS-purified T-cell subsets were activated in vitro and Th17 differentiation assessed. T-cell antigen specificities were assessed by activation with heat-killed pathogens or antigenic peptide pools. B helper capacities were determined according to antibody secretion in B-T co-cultures by ELISA. Results: CCR6+Th-cells that lacked subset-defining differentiation markers ("CCR6SP") were mostly non-polarized central memory T-cells (TCM) that produced IL-10 and expressed RORγt. They were pre-committed to a Th17 fate, since TCR stimulation in the absence of polarizing cytokines induced efficient Th17 differentiation. The latter was promoted by an autocrine loop of STAT3-activating cytokines. CCR6+Th-cells were reduced in patients with DN-STAT3 mutations but contained activated CCR6SPT-cells that produced IL-10 and responded vigorously to AD-HIES-associated pathogens. These residual CCR6+Th-cells provided B-cell help for IgG and IgE production. Conclusions: Th17 differentiation in AD-HIES patients was not completely impaired but arrested at an intermediate stage of IL-10-producing "pre-Th17"-cells. Surprisingly, DN-STAT3 mutations did not inhibit IL-10 production by CD4+T-cells. Pre-Th17-cells were activated by AD-HIES-associated pathogens and possessed B-helper functions, suggesting that they are not protective but may promote aberrant IgE production.

Autosomal Dominant Hyper-IgE Syndrome Patients Retain IL10-Producing preTh17-Cells That Are Activated by Opportunistic Pathogens and Support IgE Production / G. Moschetti, C. Vasco, F. Clemente, P. Larghi, S. Maioli, E. Scarpa, E. Carelli, N. Pulvirenti, M. Lucia Sarnicola, M. Crosti, M. Bel Imam, W. Van De Veen, L. Rizzello, S. Abrignani, L. A Baselli, R. Maria Dellepiane, M. Carrabba, G. Fabio, J. Geginat. - In: ALLERGY. - ISSN 0105-4538. - (2026), pp. 1-16. [Epub ahead of print] [10.1111/all.70266]

Autosomal Dominant Hyper-IgE Syndrome Patients Retain IL10-Producing preTh17-Cells That Are Activated by Opportunistic Pathogens and Support IgE Production

G. Moschetti
Primo
;
C. Vasco
Secondo
;
P. Larghi;S. Maioli;E. Scarpa;E. Carelli;N. Pulvirenti;L. Rizzello;S. Abrignani;M. Carrabba;G. Fabio
Penultimo
;
J. Geginat
Ultimo
2026

Abstract

Background: Autosomal Dominant-Hyper-IgE Syndrome (AD-HIES) is caused by dominant-negative (DN) STAT3 mutations and characterized by high IgE levels, a lack of Th17-cells, and recurrent infections with extracellular pathogens. We previously identified an enigmatic population of IL-10 producing CCR6+B-helper T-cells and investigated here their relationship to Th17-cells and STAT3 signaling requirements. Methods: Human blood lymphocytes were analyzed by multiparametric flow cytometry in healthy donors and AD-HIES patients. Analysis was performed by conventional gating or with bioinformatic tools. FACS-purified T-cell subsets were activated in vitro and Th17 differentiation assessed. T-cell antigen specificities were assessed by activation with heat-killed pathogens or antigenic peptide pools. B helper capacities were determined according to antibody secretion in B-T co-cultures by ELISA. Results: CCR6+Th-cells that lacked subset-defining differentiation markers ("CCR6SP") were mostly non-polarized central memory T-cells (TCM) that produced IL-10 and expressed RORγt. They were pre-committed to a Th17 fate, since TCR stimulation in the absence of polarizing cytokines induced efficient Th17 differentiation. The latter was promoted by an autocrine loop of STAT3-activating cytokines. CCR6+Th-cells were reduced in patients with DN-STAT3 mutations but contained activated CCR6SPT-cells that produced IL-10 and responded vigorously to AD-HIES-associated pathogens. These residual CCR6+Th-cells provided B-cell help for IgG and IgE production. Conclusions: Th17 differentiation in AD-HIES patients was not completely impaired but arrested at an intermediate stage of IL-10-producing "pre-Th17"-cells. Surprisingly, DN-STAT3 mutations did not inhibit IL-10 production by CD4+T-cells. Pre-Th17-cells were activated by AD-HIES-associated pathogens and possessed B-helper functions, suggesting that they are not protective but may promote aberrant IgE production.
English
IgE; T cells; immune deficiencies; interleukins;
Settore MEDS-02/B - Patologia clinica
Articolo
Esperti anonimi
Ricerca di base
Pubblicazione scientifica
   Role of innate immunity in the diverse phenotypes of Job's syndrome.
   MINISTERO DELL'UNIVERSITA' E DELLA RICERCA
   P20228W4FJ_002
2026
25-feb-2026
Wiley Blackwell Publishing : European Academy of Allergy and Clinical Immunology (EAACI)
1
16
16
Epub ahead of print
Periodico con rilevanza internazionale
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Aderisco
info:eu-repo/semantics/article
Autosomal Dominant Hyper-IgE Syndrome Patients Retain IL10-Producing preTh17-Cells That Are Activated by Opportunistic Pathogens and Support IgE Production / G. Moschetti, C. Vasco, F. Clemente, P. Larghi, S. Maioli, E. Scarpa, E. Carelli, N. Pulvirenti, M. Lucia Sarnicola, M. Crosti, M. Bel Imam, W. Van De Veen, L. Rizzello, S. Abrignani, L. A Baselli, R. Maria Dellepiane, M. Carrabba, G. Fabio, J. Geginat. - In: ALLERGY. - ISSN 0105-4538. - (2026), pp. 1-16. [Epub ahead of print] [10.1111/all.70266]
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G. Moschetti, C. Vasco, F. Clemente, P. Larghi, S. Maioli, E. Scarpa, E. Carelli, N. Pulvirenti, M. Lucia Sarnicola, M. Crosti, M. Bel Imam, W. Van De...espandi
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Utilizza questo identificativo per citare o creare un link a questo documento: https://hdl.handle.net/2434/1244572
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