白细胞介素23
银屑病
白细胞介素17
免疫系统
肿瘤坏死因子α
免疫学
白细胞介素10
医学
作者
Kazuhisa Furue,Takamichi Ito,Gaku Tsuji,Takafumi Kadono,Masutaka Furue
出处
期刊:Giornale italiano di dermatologia e venereologia
[Edizioni Minerva Medica]
日期:2019-06-01
卷期号:154 (4)
被引量:60
标识
DOI:10.23736/s0392-0488.18.06202-8
摘要
The excellent response of psoriasis to anti-TNF-α(TNF)/IL23/IL17A biologics implies a crucial role for the TNF/IL23/IL17 axis in developing psoriasis. In addition to the TNF/IL23/IL17 axis provided by immune cells, current evidence points to an important contribution of TNF, IL23 and IL17C produced from non-hematopoietic keratinocytes. Therefore, crosstalk between immune cells and keratinocytes forms a multilayered feed-forward loop to accelerate the TNF/IL23/IL17A axis. Many biologics have already been licensed or are under clinical trials. Given that the IL-17 signature is more upregulated in the skin than in synovium in psoriatic arthritis, anti-IL-23/IL-17 agents seem to be superior to anti-TNF-α remedies in the treatment of skin lesions. In this review, we summarize recent topics in psoriasis and the TNF/IL23/IL17 axis.
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