Peripherally induced RORγt<SUP>+</SUP> skin-resident regulatory T cells mediate the efficacy of allergen-specific immunotherapyPeripherally induced RORγt+ skin-resident regulatory T cells mediate the efficacy of allergen-specific immunotherapy
- Other Titles
- Peripherally induced RORγt+ skin-resident regulatory T cells mediate the efficacy of allergen-specific immunotherapy
- Authors
- Zhang, Kelun; Kim, Su Min; Kwon, Ho-Keun; Kim, Seo Hyeong; Kim, Tae-Gyun; Sun, Zhengwang; Kim, Hye Li; Tyo, Alina; Kim, Ji Hye; Kim, Ryeo Won; Kim, Jong Hoon; Choi, Je-Min; Park, Kyung Min; Kim, Lark Kyun; Sohn, Myung Hyun; Park, Jung-Won; Lee, Kwang Hoon; Kupper, Thomas S.; Park, Chang Ook
- Issue Date
- May-2025
- Publisher
- American Association for the Advancement of Science
- Citation
- Science Translational Medicine, v.17, no.800, pp 1 - 17
- Pages
- 17
- Indexed
- SCIE
SCOPUS
- Journal Title
- Science Translational Medicine
- Volume
- 17
- Number
- 800
- Start Page
- 1
- End Page
- 17
- URI
- https://scholarworks.bwise.kr/hanyang/handle/2021.sw.hanyang/207884
- DOI
- 10.1126/scitranslmed.ado1375
- ISSN
- 1946-6234
1946-6242
- Abstract
- Skin-resident regulatory T cells (Treg cells) cells play a critical role in subcutaneous allergen-specific immunotherapy (SIT) for atopic dermatitis (AD). However, a detailed description of the phenotype and origin of skin-resident Treg cells during SIT is lacking. Therefore, we investigated the role and origin of specific Treg lineages in SIT with human AD samples and with a mouse model of AD. In the blood of patients with AD who responded to SIT, Treg cells showed a notable increase in retinoic acid-related orphan receptor gamma t (ROR gamma t) expression. Moreover, ROR gamma t-expressing Treg cells expanded in the skin of patients with AD upon SIT. In a mouse model of AD, the absence of ROR gamma t expression in skin Treg cells led to reduced therapeutic efficacy with SIT. In addition, SIT-induced ROR gamma t+ Treg cells originated from peripheral tissue rather than from the thymus. Using two-photon microscopy and a parabiosis mouse model, we observed the migration and accumulation of skin-resident ROR gamma t+ Treg cells in response to the SIT-induced immune response. These findings indicate that SIT induces peripheral ROR gamma t+ Treg cell expansion, which contributes to the therapeutic efficacy of SIT.
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