Author
Listed:
- Dan Tian
(Capital Medical University
Capital Medical University
Beijing Clinical Research Institute
Beijing Key Laboratory of Tolerance Induction and Organ Protection in Transplantation)
- Lu Yang
(Capital Medical University
Beijing Clinical Research Institute
Beijing Key Laboratory of Tolerance Induction and Organ Protection in Transplantation)
- Song Wang
(Capital Medical University
Beijing Clinical Research Institute
Beijing Key Laboratory of Tolerance Induction and Organ Protection in Transplantation)
- Yanbing Zhu
(Capital Medical University
Beijing Clinical Research Institute
Beijing Key Laboratory of Tolerance Induction and Organ Protection in Transplantation)
- Wen Shi
(Capital Medical University
Beijing Clinical Research Institute
Beijing Key Laboratory of Tolerance Induction and Organ Protection in Transplantation)
- Chunpan Zhang
(Capital Medical University
Beijing Clinical Research Institute
Beijing Key Laboratory of Tolerance Induction and Organ Protection in Transplantation)
- Hua Jin
(Capital Medical University
Capital Medical University
Beijing Clinical Research Institute
Beijing Key Laboratory of Tolerance Induction and Organ Protection in Transplantation)
- Yue Tian
(Capital Medical University
Beijing Clinical Research Institute
Beijing Key Laboratory of Tolerance Induction and Organ Protection in Transplantation)
- Hufeng Xu
(Capital Medical University
Beijing Clinical Research Institute
Beijing Key Laboratory of Tolerance Induction and Organ Protection in Transplantation)
- Guangyong Sun
(Capital Medical University
Beijing Clinical Research Institute
Beijing Key Laboratory of Tolerance Induction and Organ Protection in Transplantation)
- Kai Liu
(Capital Medical University
Beijing Clinical Research Institute
Beijing Key Laboratory of Tolerance Induction and Organ Protection in Transplantation)
- Zhongtao Zhang
(Capital Medical University
Beijing Key Laboratory of Tolerance Induction and Organ Protection in Transplantation
National Clinical Research Center for Digestive Diseases)
- Dong Zhang
(Capital Medical University
Capital Medical University
Beijing Clinical Research Institute
Beijing Key Laboratory of Tolerance Induction and Organ Protection in Transplantation)
Abstract
Allergic asthma is an inflammatory disorder of the airway without satisfactory traditional therapies capable of controlling the underlying pathology. New approaches that can overcome the detrimental effects of immune dysregulation are thus desirable. Here we adoptively transfer ovalbumin (OVA) peptide-primed CD4−CD8− double negative T (DNT) cells intravenously into a mouse model of OVA-induced allergic asthma to find that OVA-induced airway hyperresponsiveness, lung inflammation, mucus production and OVA-specific IgG/IgE production are significantly suppressed. The immunosuppressive function of the OVA-specific DNT cells is dependent on the inhibition of CD11b+ dendritic cell function, T follicular helper cell proliferation, and IL-21 production. Mechanistically, Lag3 contributes to MHC-II antigen recognition and trogocytosis, thereby modulating the antigen-specific immune regulation by DNT cells. The effectiveness of ex vivo-generated allergen-specific DNT cells in alleviating airway inflammation thus supports the potential utilization of DNT cell-based therapy for the treatment of allergic asthma.
Suggested Citation
Dan Tian & Lu Yang & Song Wang & Yanbing Zhu & Wen Shi & Chunpan Zhang & Hua Jin & Yue Tian & Hufeng Xu & Guangyong Sun & Kai Liu & Zhongtao Zhang & Dong Zhang, 2019.
"Double negative T cells mediate Lag3-dependent antigen-specific protection in allergic asthma,"
Nature Communications, Nature, vol. 10(1), pages 1-13, December.
Handle:
RePEc:nat:natcom:v:10:y:2019:i:1:d:10.1038_s41467-019-12243-0
DOI: 10.1038/s41467-019-12243-0
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