STING-STAT6 Signaling Pathway Promotes IL-4+and IFN-α plus Fibrotic T Cell Activation and Exacerbates Scleroderma in SKG MiceSTING-STAT6 Signaling Pathway Promotes IL-4+ and IFN-α+ Fibrotic T Cell Activation and Exacerbates Scleroderma in SKG Mice
- Other Titles
- STING-STAT6 Signaling Pathway Promotes IL-4+ and IFN-α+ Fibrotic T Cell Activation and Exacerbates Scleroderma in SKG Mice
- Authors
- Lee, Kun Hee; Woo, Jin Seok; Jeong, Ha Yeon; Choi, Jeong Won; Bang, Chul Hwan; Youn, Jeehee; Park, Sung-Hwan; Cho, Mi-La
- Issue Date
- Oct-2024
- Publisher
- 대한면역학회
- Keywords
- Systemic sclerosis; T cell; STING; STAT6 transcription factor; Cytokine
- Citation
- Immune Network, v.24, no.5, pp 1 - 17
- Pages
- 17
- Indexed
- SCIE
SCOPUS
KCI
- Journal Title
- Immune Network
- Volume
- 24
- Number
- 5
- Start Page
- 1
- End Page
- 17
- URI
- https://scholarworks.bwise.kr/hanyang/handle/2021.sw.hanyang/210161
- DOI
- 10.4110/in.2024.24.e37
- ISSN
- 1598-2629
2092-6685
- Abstract
- Systemic sclerosis (SS) is an autoimmune disease and pathological mechanisms of SS are unclear. In this study, we investigated the role of T cells in the progression of SS using SKG mice and humanized mice. SKG mice have a spontaneous point mutation in ZAP70. We induced scleroderma in SKG mice and a humanized SS mouse model to assess whether T cell-mediated immune responses induce SS. As a result, we found increased dermal thickness, fibrosis, and lymphocyte infiltration in skin tissue in SKG SS mice compared to BALB/c mice (control). Also, blood cytokine level, including IL-4- and IFN-α which are produced by CD4+ T cells via STIM1/STING/STAT6/IRF3 signaling pathways, were increased in SKG mice. Interestingly, skin fibrosis was reduced by inhibiting STING pathway in skin fibroblast. Next, we demonstrated the pathophysiological role of IL-4 and IFN-α in skin fibrosis using a humanized SS mouse model and found increased IL-4- and IFN-α-producing CD4+ T cells and fibrosis. In this study, we found that STING-induced production of IL-4- and type I IFN by CD4+ T cells is a key factor in mouse model and humanized mouse model of SS. Our findings suggest that the STING/STAT6/IRF3 signaling pathways are potential therapeutic targets in SS.
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