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Programmed cell death ligand 1 alleviates psoriatic inflammation by suppressing IL-17A production from programmed cell death 1-high T cells.
DC Field | Value | Language |
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dc.contributor.author | 김송이 | - |
dc.contributor.author | 김수찬 | - |
dc.contributor.author | 김형표 | - |
dc.contributor.author | 김종훈 | - |
dc.date.accessioned | 2017-02-27T07:55:59Z | - |
dc.date.available | 2017-02-27T07:55:59Z | - |
dc.date.issued | 2016 | - |
dc.identifier.issn | 0091-6749 | - |
dc.identifier.uri | https://ir.ymlib.yonsei.ac.kr/handle/22282913/147037 | - |
dc.description.abstract | BACKGROUND: Psoriasis is one of the most common chronic inflammatory diseases of the skin. Recently, IL-17-producing T cells have been shown to play a critical role in psoriatic inflammation. Programmed cell death 1 (PD-1) is a coinhibitory receptor expressed on T cells in various chronic inflammatory diseases; however, the expression and function of PD-1 during psoriatic inflammation have not previously been characterized. OBJECTIVE: We examined PD-1 expression on IL-17A-producing T cells from imiquimod-treated mice and patients with psoriasis. Additionally, we investigated the therapeutic effect of recombinant programmed cell death ligand 1 (PD-L1) protein on imiquimod-induced psoriatic inflammation. METHODS: PD-1 expression on IL-17A-producing γδ T cells from imiquimod-treated mice was examined by means of multicolor flow cytometric analysis. In the psoriatic skin of patients, PD-1 and IL-17A expression was analyzed by using immunofluorescence. The therapeutic effect of PD-L1-Fc fusion protein (PD-L1-Fc) was assessed in imiquimod-treated mice ex vivo and in vivo. RESULTS: During imiquimod-induced psoriatic inflammation, PD-1 is overexpressed on CD27(-)Vγ1(-) γδ T cells. Furthermore, PD-1 expression on IL-17A(+) T cells was confirmed in psoriatic skin tissues from patients and imiquimod-treated mice. In the CD27(-)Vγ1(-) γδ T-cell population, Vγ4(-) γδ T cells with Vγ6 mRNA expression showed a high level of PD-1 expression. Furthermore, these PD-1(hi)Vγ4(-) (Vγ6(+)) γδ T cells were specialized for anti-CD3-induced IL-17A production, which was inhibited by PD-L1-Fc treatment. In imiquimod-treated mice PD-L1-Fc reduced psoriatic inflammation when given alone and enhanced the therapeutic effect of anti-p40 when given in combination. CONCLUSION: PD-1 is overexpressed in IL-17A-producing T cells in both imiquimod-treated mice and patients with psoriasis. Moreover, recombinant PD-L1-Fc alleviates psoriatic inflammation in imiquimod-treated mice. | - |
dc.description.statementOfResponsibility | restriction | - |
dc.format.extent | 1466~1476 | - |
dc.language | English | - |
dc.publisher | St Louis, Mosby | - |
dc.relation.isPartOf | JOURNAL OF ALLERGY AND CLINICAL IMMUNOLOGY | - |
dc.rights | CC BY-NC-ND 2.0 KR | - |
dc.rights.uri | https://creativecommons.org/licenses/by-nc-nd/2.0/kr/ | - |
dc.subject.MESH | Adjuvants, Immunologic | - |
dc.subject.MESH | Aminoquinolines | - |
dc.subject.MESH | Animals | - |
dc.subject.MESH | B7-H1 Antigen/pharmacology | - |
dc.subject.MESH | B7-H1 Antigen/therapeutic use | - |
dc.subject.MESH | Humans | - |
dc.subject.MESH | Inflammation/metabolism | - |
dc.subject.MESH | Interleukin-17/metabolism* | - |
dc.subject.MESH | Mice, Inbred C57BL | - |
dc.subject.MESH | Programmed Cell Death 1 Receptor/metabolism* | - |
dc.subject.MESH | Psoriasis/chemically induced | - |
dc.subject.MESH | Psoriasis/drug therapy | - |
dc.subject.MESH | Psoriasis/metabolism* | - |
dc.subject.MESH | Recombinant Proteins/pharmacology | - |
dc.subject.MESH | Recombinant Proteins/therapeutic use | - |
dc.subject.MESH | Skin/drug effects | - |
dc.subject.MESH | Skin/metabolism | - |
dc.subject.MESH | T-Lymphocyte Subsets/metabolism* | - |
dc.title | Programmed cell death ligand 1 alleviates psoriatic inflammation by suppressing IL-17A production from programmed cell death 1-high T cells. | - |
dc.type | Article | - |
dc.publisher.location | United States | - |
dc.contributor.college | College of Medicine | - |
dc.contributor.department | Yonsei Biomedical Research Center | - |
dc.contributor.googleauthor | Jong Hoon Kim | - |
dc.contributor.googleauthor | Young Joon Choi | - |
dc.contributor.googleauthor | Byung Ha Lee | - |
dc.contributor.googleauthor | Mi-Young Song | - |
dc.contributor.googleauthor | Chae Yeon Ban | - |
dc.contributor.googleauthor | Jihye Kim | - |
dc.contributor.googleauthor | Junsik Park | - |
dc.contributor.googleauthor | Song-Ee Kim | - |
dc.contributor.googleauthor | Tae-Gyun Kim | - |
dc.contributor.googleauthor | Su-Hyung Park | - |
dc.contributor.googleauthor | Hyoung-Pyo Kim | - |
dc.contributor.googleauthor | Young-Chul Sung | - |
dc.contributor.googleauthor | Soo-Chan Kim | - |
dc.contributor.googleauthor | Eui-Cheol Shin | - |
dc.identifier.doi | 10.1016/j.jaci.2015.11.021 | - |
dc.contributor.localId | A00627 | - |
dc.contributor.localId | A00637 | - |
dc.contributor.localId | A01163 | - |
dc.contributor.localId | A05233 | - |
dc.relation.journalcode | J01228 | - |
dc.identifier.eissn | 1097-6825 | - |
dc.identifier.pmid | 26824999 | - |
dc.identifier.url | http://www.sciencedirect.com/science/article/pii/S0091674916000221 | - |
dc.subject.keyword | IL-17A | - |
dc.subject.keyword | Psoriasis | - |
dc.subject.keyword | T cell | - |
dc.subject.keyword | programmed cell death 1 | - |
dc.subject.keyword | programmed cell death ligand 1 | - |
dc.contributor.alternativeName | Kim, Song Ee | - |
dc.contributor.alternativeName | Kim, Soo Chan | - |
dc.contributor.alternativeName | Kim, Hyoung Pyo | - |
dc.contributor.affiliatedAuthor | Kim, Song Ee | - |
dc.contributor.affiliatedAuthor | Kim, Soo Chan | - |
dc.contributor.affiliatedAuthor | Kim, Hyoung Pyo | - |
dc.contributor.affiliatedAuthor | Kim, Jong Hoon | - |
dc.citation.volume | 137 | - |
dc.citation.number | 5 | - |
dc.citation.startPage | 1466 | - |
dc.citation.endPage | 1476 | - |
dc.identifier.bibliographicCitation | JOURNAL OF ALLERGY AND CLINICAL IMMUNOLOGY, Vol.137(5) : 1466-1476, 2016 | - |
dc.date.modified | 2017-02-24 | - |
dc.identifier.rimsid | 47069 | - |
dc.type.rims | ART | - |
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