Macrophage‐derived progranulin promotes allergen‐induced airway inflammation

Background Progranulin (PGRN), mainly produced by immune and epithelial cells, has been known to be involved in the development of various inflammatory diseases. However, the function of PGRN in allergic airway inflammation has not been clearly elucidated, and we investigated the role of PGRN in all...

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Published in:	Allergy (Copenhagen) Vol. 75; no. 5; pp. 1133 - 1145
Main Authors:	Choi, Jun‐Pyo, Park, So Young, Moon, Keun‐Ai, Ha, Eun Hee, Woo, Yeon Duk, Chung, Doo Hyun, Kwon, Hyouk‐Soo, Kim, Tae‐Bum, Park, Hae‐Sim, Moon, Hee‐Bom, Song, Woo‐Jung, Cho, You Sook
Format:	Journal Article
Language:	English
Published:	Denmark Blackwell Publishing Ltd 01-05-2020
Subjects:	airway Allergens Allergies Alveoli Animal models Animals Asthma Bronchus Cell lines Cytokines Disease Models, Animal Epithelial cells house dust mite Hypersensitivity Hypersensitivity - immunology Immune response Inflammation Inflammatory diseases Lymphocytes T macrophage Macrophages Mice Natural killer cells progranulin Progranulins Pyroglyphidae Respiratory tract Respiratory tract diseases Rodents Th2 Cells Thymic stromal lymphopoietin progranulin macrophage house dust mite inflammation airway
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Abstract	Background Progranulin (PGRN), mainly produced by immune and epithelial cells, has been known to be involved in the development of various inflammatory diseases. However, the function of PGRN in allergic airway inflammation has not been clearly elucidated, and we investigated the role of PGRN in allergic airway inflammation. Methods Production of PGRN and various type 2 cytokines was evaluated in mouse airways exposed to house dust mite allergen, and main cellular sources of these molecules were investigated using macrophage, airway epithelial cell, and NKT cell lines. We elucidated the role of PGRN in allergic airway inflammation in mouse models of asthma using macrophage‐derived PGRN‐deficient mice and NKT cell knockout mice by evaluating cytokine levels in bronchoalveolar lavage fluids and histopathology. We also supplemented recombinant PGRN in the mouse models to confirm the role of PGRN in allergic airway inflammation. Results PGRN production preceded other cytokines, mainly from macrophages, in the airway exposed to allergen. PGRN induced IL‐4 and IL‐13 production in NKT cells and IL‐33 and TSLP in airway epithelial cells. PGRN‐induced Th2 cytokine production was abolished in NKT‐deficient mice. Finally, allergic inflammation was significantly attenuated in allergen‐exposed PGRN‐deficient mice, but inflammation was restored when recombinant PGRN was supplemented during the allergen sensitization period. Conclusion The presence of macrophage‐derived PGRN in airways in the early sensitization period may be critical for mounting a Th2 immune response and for following an allergic airway inflammation pathway via induction of type 2 cytokine production in NKT and airway epithelial cells. During allergen sensitization, PGRN, produced mainly from alveolar macrophages, induces type 2 cytokines (IL‐4, IL‐13, IL‐33, and TSLP) via NKT cells and lung epithelial cells. The absence of alveolar macrophage‐derived PGRN or NKT cells in sensitization period induces downregulation of type 2 cytokines and development of allergen‐specific Th2 airway inflammation. Abbreviations: PGRN, progranulin; TSLP, thymic stromal lymphopoietin
AbstractList	Progranulin (PGRN), mainly produced by immune and epithelial cells, has been known to be involved in the development of various inflammatory diseases. However, the function of PGRN in allergic airway inflammation has not been clearly elucidated, and we investigated the role of PGRN in allergic airway inflammation. Production of PGRN and various type 2 cytokines was evaluated in mouse airways exposed to house dust mite allergen, and main cellular sources of these molecules were investigated using macrophage, airway epithelial cell, and NKT cell lines. We elucidated the role of PGRN in allergic airway inflammation in mouse models of asthma using macrophage-derived PGRN-deficient mice and NKT cell knockout mice by evaluating cytokine levels in bronchoalveolar lavage fluids and histopathology. We also supplemented recombinant PGRN in the mouse models to confirm the role of PGRN in allergic airway inflammation. PGRN production preceded other cytokines, mainly from macrophages, in the airway exposed to allergen. PGRN induced IL-4 and IL-13 production in NKT cells and IL-33 and TSLP in airway epithelial cells. PGRN-induced Th2 cytokine production was abolished in NKT-deficient mice. Finally, allergic inflammation was significantly attenuated in allergen-exposed PGRN-deficient mice, but inflammation was restored when recombinant PGRN was supplemented during the allergen sensitization period. The presence of macrophage-derived PGRN in airways in the early sensitization period may be critical for mounting a Th2 immune response and for following an allergic airway inflammation pathway via induction of type 2 cytokine production in NKT and airway epithelial cells. Background Progranulin (PGRN), mainly produced by immune and epithelial cells, has been known to be involved in the development of various inflammatory diseases. However, the function of PGRN in allergic airway inflammation has not been clearly elucidated, and we investigated the role of PGRN in allergic airway inflammation. Methods Production of PGRN and various type 2 cytokines was evaluated in mouse airways exposed to house dust mite allergen, and main cellular sources of these molecules were investigated using macrophage, airway epithelial cell, and NKT cell lines. We elucidated the role of PGRN in allergic airway inflammation in mouse models of asthma using macrophage‐derived PGRN‐deficient mice and NKT cell knockout mice by evaluating cytokine levels in bronchoalveolar lavage fluids and histopathology. We also supplemented recombinant PGRN in the mouse models to confirm the role of PGRN in allergic airway inflammation. Results PGRN production preceded other cytokines, mainly from macrophages, in the airway exposed to allergen. PGRN induced IL‐4 and IL‐13 production in NKT cells and IL‐33 and TSLP in airway epithelial cells. PGRN‐induced Th2 cytokine production was abolished in NKT‐deficient mice. Finally, allergic inflammation was significantly attenuated in allergen‐exposed PGRN‐deficient mice, but inflammation was restored when recombinant PGRN was supplemented during the allergen sensitization period. Conclusion The presence of macrophage‐derived PGRN in airways in the early sensitization period may be critical for mounting a Th2 immune response and for following an allergic airway inflammation pathway via induction of type 2 cytokine production in NKT and airway epithelial cells. During allergen sensitization, PGRN, produced mainly from alveolar macrophages, induces type 2 cytokines (IL‐4, IL‐13, IL‐33, and TSLP) via NKT cells and lung epithelial cells. The absence of alveolar macrophage‐derived PGRN or NKT cells in sensitization period induces downregulation of type 2 cytokines and development of allergen‐specific Th2 airway inflammation. Abbreviations: PGRN, progranulin; TSLP, thymic stromal lymphopoietin BACKGROUNDProgranulin (PGRN), mainly produced by immune and epithelial cells, has been known to be involved in the development of various inflammatory diseases. However, the function of PGRN in allergic airway inflammation has not been clearly elucidated, and we investigated the role of PGRN in allergic airway inflammation. METHODSProduction of PGRN and various type 2 cytokines was evaluated in mouse airways exposed to house dust mite allergen, and main cellular sources of these molecules were investigated using macrophage, airway epithelial cell, and NKT cell lines. We elucidated the role of PGRN in allergic airway inflammation in mouse models of asthma using macrophage-derived PGRN-deficient mice and NKT cell knockout mice by evaluating cytokine levels in bronchoalveolar lavage fluids and histopathology. We also supplemented recombinant PGRN in the mouse models to confirm the role of PGRN in allergic airway inflammation. RESULTSPGRN production preceded other cytokines, mainly from macrophages, in the airway exposed to allergen. PGRN induced IL-4 and IL-13 production in NKT cells and IL-33 and TSLP in airway epithelial cells. PGRN-induced Th2 cytokine production was abolished in NKT-deficient mice. Finally, allergic inflammation was significantly attenuated in allergen-exposed PGRN-deficient mice, but inflammation was restored when recombinant PGRN was supplemented during the allergen sensitization period. CONCLUSIONThe presence of macrophage-derived PGRN in airways in the early sensitization period may be critical for mounting a Th2 immune response and for following an allergic airway inflammation pathway via induction of type 2 cytokine production in NKT and airway epithelial cells.
Author	Chung, Doo Hyun Song, Woo‐Jung Kim, Tae‐Bum Choi, Jun‐Pyo Moon, Keun‐Ai Ha, Eun Hee Woo, Yeon Duk Kwon, Hyouk‐Soo Park, Hae‐Sim Park, So Young Moon, Hee‐Bom Cho, You Sook
Author_xml	– sequence: 1 givenname: Jun‐Pyo orcidid: 0000-0001-8925-1786 surname: Choi fullname: Choi, Jun‐Pyo organization: University of Ulsan College of Medicine – sequence: 2 givenname: So Young surname: Park fullname: Park, So Young organization: Eulji University School of Medicine – sequence: 3 givenname: Keun‐Ai surname: Moon fullname: Moon, Keun‐Ai organization: University of Ulsan College of Medicine – sequence: 4 givenname: Eun Hee surname: Ha fullname: Ha, Eun Hee organization: University of Ulsan College of Medicine – sequence: 5 givenname: Yeon Duk surname: Woo fullname: Woo, Yeon Duk organization: Seoul National University Medical Research Center – sequence: 6 givenname: Doo Hyun surname: Chung fullname: Chung, Doo Hyun organization: Seoul National University Medical Research Center – sequence: 7 givenname: Hyouk‐Soo surname: Kwon fullname: Kwon, Hyouk‐Soo organization: University of Ulsan College of Medicine – sequence: 8 givenname: Tae‐Bum orcidid: 0000-0001-5663-0640 surname: Kim fullname: Kim, Tae‐Bum organization: University of Ulsan College of Medicine – sequence: 9 givenname: Hae‐Sim orcidid: 0000-0003-2614-0303 surname: Park fullname: Park, Hae‐Sim organization: Ajou University School of Medicine – sequence: 10 givenname: Hee‐Bom surname: Moon fullname: Moon, Hee‐Bom organization: University of Ulsan College of Medicine – sequence: 11 givenname: Woo‐Jung orcidid: 0000-0002-4630-9922 surname: Song fullname: Song, Woo‐Jung organization: University of Ulsan College of Medicine – sequence: 12 givenname: You Sook surname: Cho fullname: Cho, You Sook email: yscho@amc.seoul.kr organization: University of Ulsan College of Medicine
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Snippet	Background Progranulin (PGRN), mainly produced by immune and epithelial cells, has been known to be involved in the development of various inflammatory... Progranulin (PGRN), mainly produced by immune and epithelial cells, has been known to be involved in the development of various inflammatory diseases. However,... BackgroundProgranulin (PGRN), mainly produced by immune and epithelial cells, has been known to be involved in the development of various inflammatory... BACKGROUNDProgranulin (PGRN), mainly produced by immune and epithelial cells, has been known to be involved in the development of various inflammatory...
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SubjectTerms	airway Allergens Allergies Alveoli Animal models Animals Asthma Bronchus Cell lines Cytokines Disease Models, Animal Epithelial cells house dust mite Hypersensitivity Hypersensitivity - immunology Immune response Inflammation Inflammatory diseases Lymphocytes T macrophage Macrophages Mice Natural killer cells progranulin Progranulins Pyroglyphidae Respiratory tract Respiratory tract diseases Rodents Th2 Cells Thymic stromal lymphopoietin
Title	Macrophage‐derived progranulin promotes allergen‐induced airway inflammation
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