Literature DB >> 30194239

Inception of early-life allergen-induced airway hyperresponsiveness is reliant on IL-13+CD4+ T cells.

Sejal Saglani1,2, Lisa G Gregory3, Avneet K Manghera3, William J Branchett3, Faith Uwadiae3, Lewis J Entwistle3, R A Oliver3, Jessica E Vasiliou3, Rebekah Sherburn3, Stephen Lui3, F Puttur3, David Vöhringer4, Simone A Walker3, James Buckley3, Ruth Grychtol3, Valentina Fainardi3, Laura Denney3, Adam Byrne3, Erika von Mutius5, Andrew Bush2, Clare M Lloyd1.   

Abstract

Airway hyperresponsiveness (AHR) is a critical feature of wheezing and asthma in children, but the initiating immune mechanisms remain unconfirmed. We demonstrate that both recombinant interleukin-33 (rIL-33) and allergen [house dust mite (HDM) or Alternaria alternata] exposure from day 3 of life resulted in significantly increased pulmonary IL-13+CD4+ T cells, which were indispensable for the development of AHR. In contrast, adult mice had a predominance of pulmonary LinnegCD45+CD90+IL-13+ type 2 innate lymphoid cells (ILC2s) after administration of rIL-33. HDM exposure of neonatal IL-33 knockout (KO) mice still resulted in AHR. However, neonatal CD4creIL-13 KO mice (lacking IL-13+CD4+ T cells) exposed to allergen from day 3 of life were protected from AHR despite persistent pulmonary eosinophilia, elevated IL-33 levels, and IL-13+ ILCs. Moreover, neonatal mice were protected from AHR when inhaled Acinetobacter lwoffii (an environmental bacterial isolate found in cattle farms, which is known to protect from childhood asthma) was administered concurrent with HDM. A. lwoffii blocked the expansion of pulmonary IL-13+CD4+ T cells, whereas IL-13+ ILCs and IL-33 remained elevated. Administration of A. lwoffii mirrored the findings from the CD4creIL-13 KO mice, providing a translational approach for disease protection in early life. These data demonstrate that IL-13+CD4+ T cells, rather than IL-13+ ILCs or IL-33, are critical for inception of allergic AHR in early life.
Copyright © 2018 The Authors, some rights reserved; exclusive licensee American Association for the Advancement of Science. No claim to original U.S. Government Works.

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Year:  2018        PMID: 30194239      PMCID: PMC7613599          DOI: 10.1126/sciimmunol.aan4128

Source DB:  PubMed          Journal:  Sci Immunol        ISSN: 2470-9468


  52 in total

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6.  The significance of early recurrent wheeze for asthma outcomes in late childhood.

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7.  Innate Immunity and Asthma Risk in Amish and Hutterite Farm Children.

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10.  First-Breath-Induced Type 2 Pathways Shape the Lung Immune Environment.

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Review 7.  T cells in severe childhood asthma.

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Review 9.  The allergenic activity and clinical impact of individual IgE-antibody binding molecules from indoor allergen sources.

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10.  Analysis of Results of Specific IgE in 100 Atopic Dermatitis Patients with the Use of Multiplex Examination ALEX2-Allergy Explorer.

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