| Literature DB >> 28002730 |
Etsushi Kuroda1, Koji Ozasa2, Burcu Temizoz3, Keiichi Ohata3, Christine X Koo4, Tomohiro Kanuma5, Takato Kusakabe5, Shingo Kobari2, Masanori Horie6, Yasuo Morimoto7, Saeko Nakajima8, Kenji Kabashima8, Steven F Ziegler9, Yoichiro Iwakura10, Wataru Ise11, Tomohiro Kurosaki11, Takahiro Nagatake12, Jun Kunisawa12, Naoki Takemura13, Satoshi Uematsu13, Masayuki Hayashi14, Taiki Aoshi15, Kouji Kobiyama16, Cevayir Coban17, Ken J Ishii18.
Abstract
Particulate pollution is thought to function as an adjuvant that can induce allergic responses. However, the exact cell types and immunological factors that initiate the lung-specific immune responses are unclear. We found that upon intratracheal instillation, particulates such as aluminum salts and silica killed alveolar macrophages (AMs), which then released interleukin-1α (IL-1α) and caused inducible bronchus-associated lymphoid tissue (iBALT) formation in the lung. IL-1α release continued for up to 2 weeks after particulate exposure, and type-2 allergic immune responses were induced by the inhalation of antigen during IL-1α release and iBALT formation, even long after particulate instillation. Recombinant IL-1α was sufficient to induce iBALTs, which coincided with subsequent immunoglobulin E responses, and IL-1-receptor-deficient mice failed to induce iBALT formation. Therefore, the AM-IL-1α-iBALT axis might be a therapeutic target for particulate-induced allergic inflammation.Entities:
Keywords: IL-1α; IgE; Particulate; alveolar macrophages; iBALT
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Year: 2016 PMID: 28002730 DOI: 10.1016/j.immuni.2016.11.010
Source DB: PubMed Journal: Immunity ISSN: 1074-7613 Impact factor: 31.745