Human T
| Autor: | Holliday T. Carper, Lyndsey M. Muehling, Brian J. Capaldo, William W. Kwok, Judith A. Woodfolk, Deborah D. Murphy, Lisa J. Workman, Ronald B. Turner, Rachana Agrawal, Sarah J. Ratcliffe, Thomas Ae Platts-Mills, Jacob D. Eccles, Peter W. Heymann, Paul W. Wright, Carolyn R. Word |
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| Rok vydání: | 2019 |
| Předmět: |
0301 basic medicine
Allergy Rhinovirus Immunology Programmed Cell Death 1 Receptor Plasmacytoid dendritic cell medicine.disease_cause Immunoglobulin E Lymphocyte Activation Article 03 medical and health sciences FEV1/FVC ratio 0302 clinical medicine Allergen Th2 Cells medicine Hypersensitivity Immunology and Allergy Humans Antigens Viral Cells Cultured Asthma Respiratory Sounds Innate immune system Picornaviridae Infections biology business.industry respiratory system Allergens Th1 Cells medicine.disease 030104 developmental biology 030228 respiratory system biology.protein Cytokines Disease Susceptibility business |
| Zdroj: | J Allergy Clin Immunol |
| ISSN: | 1097-6825 |
| Popis: | Background Allergic asthmatic subjects are uniquely susceptible to acute wheezing episodes provoked by rhinovirus. However, the underlying immune mechanisms and interaction between rhinovirus and allergy remain enigmatic, and current paradigms are controversial. Objective We sought to perform a comprehensive analysis of type 1 and type 2 innate and adaptive responses in allergic asthmatic subjects infected with rhinovirus. Methods Circulating virus-specific TH1 cells and allergen-specific TH2 cells were precisely monitored before and after rhinovirus challenge in allergic asthmatic subjects (total IgE, 133-4692 IU/mL; n = 28) and healthy nonallergic controls (n = 12) using peptide/MHCII tetramers. T cells were sampled for up to 11 weeks to capture steady-state and postinfection phases. T-cell responses were analyzed in parallel with 18 cytokines in the nose, upper and lower airway symptoms, and lung function. The influence of in vivo IgE blockade was also examined. Results In uninfected asthmatic subjects, higher numbers of circulating virus-specific PD-1+ TH1 cells, but not allergen-specific TH2 cells, were linked to worse lung function. Rhinovirus infection induced an amplified antiviral TH1 response in asthmatic subjects versus controls, with synchronized allergen-specific TH2 expansion, and production of type 1 and 2 cytokines in the nose. In contrast, TH2 responses were absent in infected asthmatic subjects who had normal lung function, and in those receiving anti-IgE. Across all subjects, early induction of a minimal set of nasal cytokines that discriminated high responders (G-CSF, IFN-γ, TNF-α) correlated with both egress of circulating virus-specific TH1 cells and worse symptoms. Conclusions Rhinovirus induces robust TH1 responses in allergic asthmatic subjects that may promote disease, even after the infection resolves. |
| Databáze: | OpenAIRE |
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