Inflammatory and tolerogenic myeloid cells determine outcome following human allergen challenge

Author:

Voskamp Astrid L.1ORCID,Tak Tamar1ORCID,Gerdes Maarten L.2ORCID,Menafra Roberta3ORCID,Duijster Ellen4ORCID,Jochems Simon P.1ORCID,Kielbasa Szymon M.5ORCID,Kormelink Tom Groot6ORCID,Stam Koen A.1ORCID,van Hengel Oscar R.J.1ORCID,de Jong Nicolette W.4ORCID,Hendriks Rudi W.7ORCID,Kloet Susan L.3ORCID,Yazdanbakhsh Maria1ORCID,de Jong Esther C.6ORCID,Gerth van Wijk Roy4ORCID,Smits Hermelijn H.1ORCID

Affiliation:

1. Leiden University Medical Center 1 Department of Parasitology, , Leiden, Netherlands

2. Erasmus University Medical Center 2 Department of Ear, Nose and Throat, , Rotterdam, Netherlands

3. Leiden Genome Technology Center, Leiden University Medical Center 3 , Leiden, Netherlands

4. Department of Internal Medicine, Section Allergology and Clinical Immunology, Erasmus University Medical Center 4 , Rotterdam, Netherlands

5. Leiden University Medical Center 5 Department of Biomedical Data Sciences, , Leiden, Netherlands

6. Amsterdam University Medical Centers 6 Department of Exp Immunology, , Amsterdam, Netherlands

7. Erasmus University Medical Center 7 Department of Pulmonary Medicine, , Rotterdam, Netherlands

Abstract

Innate mononuclear phagocytic system (MPS) cells preserve mucosal immune homeostasis. We investigated their role at nasal mucosa following allergen challenge with house dust mite. We combined single-cell proteome and transcriptome profiling on nasal immune cells from nasal biopsies cells from 30 allergic rhinitis and 27 non-allergic subjects before and after repeated nasal allergen challenge. Biopsies of patients showed infiltrating inflammatory HLA-DRhi/CD14+ and CD16+ monocytes and proallergic transcriptional changes in resident CD1C+/CD1A+ conventional dendritic cells (cDC)2 following challenge. In contrast, non-allergic individuals displayed distinct innate MPS responses to allergen challenge: predominant infiltration of myeloid-derived suppressor cells (MDSC: HLA-DRlow/CD14+ monocytes) and cDC2 expressing inhibitory/tolerogenic transcripts. These divergent patterns were confirmed in ex vivo stimulated MPS nasal biopsy cells. Thus, we identified not only MPS cell clusters involved in airway allergic inflammation but also highlight novel roles for non-inflammatory innate MPS responses by MDSC to allergens in non-allergic individuals. Future therapies should address MDSC activity as treatment for inflammatory airway diseases.

Funder

Netherlands Lung Foundation

LSH-TKI

Netherlands Science Council

Publisher

Rockefeller University Press

Subject

Immunology,Immunology and Allergy

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