白细胞介素23
医学
乌斯特基努马
体内
银屑病
免疫学
单克隆抗体
药理学
抗体
白细胞介素17
免疫系统
生物
肿瘤坏死因子α
生物技术
英夫利昔单抗
作者
Li Zhou,Yibing Wang,Qi Wan,Fei Wu,Jeffrey Barbon,Robert W. Dunstan,Stephen B. Gauld,Mark A. P. Konrad,Laura Leys,Richard McCarthy,Marian T. Namovic,Christine M. Nelson,Gary Overmeyer,Denise Perron,Zhi Su,Leyu Wang,Susan V. Westmoreland,Jun Zhang,Rui Zhu,Geertruida M. Veldman
出处
期刊:mAbs
[Landes Bioscience]
日期:2021-01-01
卷期号:13 (1): 1964420-1964420
被引量:52
标识
DOI:10.1080/19420862.2021.1964420
摘要
Four antibodies that inhibit interleukin (IL)-23 are approved for the treatment of moderate-to-severe plaque psoriasis. Here, we present non-clinical data comparing ustekinumab, guselkumab, tildrakizumab and risankizumab with regard to thermostability, IL-23 binding affinity, inhibitory-binding mode, in vitro potency and in vivo efficacy. Risankizumab and guselkumab exhibited 5-fold higher affinity for IL-23 and showed more potent inhibition of IL-23 signaling than ustekinumab and tildrakizumab. Risankizumab and guselkumab completely blocked the binding of IL-23 to IL-23Rα as expected, whereas tildrakizumab did not. In vitro, risankizumab and guselkumab blocked the terminal differentiation of TH17 cells in a similar manner, while tildrakizumab had minimal impact on TH17 differentiation. In a human IL-23-induced ear-swelling mouse model, risankizumab and guselkumab were more effective than ustekinumab and tildrakizumab at reducing IL-17, IL-22, and keratinocyte gene expression. Our results indicate that the four clinically approved antibodies targeting IL-23 differ in affinity and binding epitope. These attributes contribute to differences in in vitro potency, receptor interaction inhibition mode and in vivo efficacy in preclinical studies as described in this report, and similarly may affect the clinical performance of these drugs.
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