Stat3 as a potential therapeutic target for rheumatoid arthritis

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作者
Takatsugu Oike
Yuiko Sato
Tami Kobayashi
Kana Miyamoto
Satoshi Nakamura
Yosuke Kaneko
Shu Kobayashi
Kengo Harato
Hideyuki Saya
Morio Matsumoto
Masaya Nakamura
Yasuo Niki
Takeshi Miyamoto
机构
[1] Department of Orthopedic Surgery,
[2] Keio University School of Medicine,undefined
[3] 35 Shinano-machi,undefined
[4] Shinjuku-ku,undefined
[5] Department of Advanced Therapy for Musculoskeletal Disorders,undefined
[6] Keio University School of Medicine,undefined
[7] 35 Shinano-machi,undefined
[8] Shinjuku-ku,undefined
[9] Department of Musculoskeletal Reconstruction and Regeneration Surgery,undefined
[10] Keio University School of Medicine,undefined
[11] 35 Shinano-machi,undefined
[12] Shinjuku-ku,undefined
[13] Division of Gene Regulation,undefined
[14] Institute for Advanced Medical Research,undefined
[15] Keio University School of Medicine,undefined
[16] 35 Shinano-machi,undefined
[17] Shinjuku-ku,undefined
来源
Scientific Reports | / 7卷
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摘要
Rheumatoid arthritis (RA) is a multi-factorial disease characterized by chronic inflammation and destruction of multiple joints. To date, various biologic treatments for RA such as anti-tumor necrosis factor alpha antibodies have been developed; however, mechanisms underlying RA development remain unclear and targeted therapy for this condition has not been established. Here, we provide evidence that signal transducer and activator of transcription 3 (Stat3) promotes inflammation and joint erosion in a mouse model of arthritis. Stat3 global KO mice show early embryonic lethality; thus, we generated viable Stat3 conditional knockout adult mice and found that they were significantly resistant to collagen-induced arthritis (CIA), the most common RA model, compared with controls. We then used an in vitro culture system to screen ninety-six existing drugs to select Stat3 inhibitors and selected five candidate inhibitors. Among them, three significantly inhibited development of arthritis and joint erosion in CIA wild-type mice. These findings suggest that Stat3 inhibitors may serve as promising drugs for RA therapy.
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