JAK 选择性及其对 filgotinib、upadacitinib、tofacitinib 和 baricitinib 抑制药效细胞因子信号的临床意义。
JAK selectivity and the implications for clinical inhibition of pharmacodynamic cytokine signalling by filgotinib, upadacitinib, tofacitinib and baricitinib.
机构信息
Inflammation Biology, Gilead Sciences, Foster City, California, USA.
Drug Metabolism, Gilead Sciences, Foster City, California, USA.
出版信息
Ann Rheum Dis. 2021 Jul;80(7):865-875. doi: 10.1136/annrheumdis-2020-219012. Epub 2021 Mar 19.
OBJECTIVE
Janus kinase inhibitors (JAKinibs) are efficacious in rheumatoid arthritis (RA) with variable reported rates of adverse events, potentially related to differential JAK family member selectivity. Filgotinib was compared with baricitinib, tofacitinib and upadacitinib to elucidate the pharmacological basis underlying its clinical efficacy and safety.
METHODS
In vitro JAKinib inhibition of signal transducer and activator of transcription phosphorylation (pSTAT) was measured by flow cytometry in peripheral blood mononuclear cells and whole blood from healthy donors and patients with RA following cytokine stimulation of distinct JAK/STAT pathways. The average daily pSTAT and time above 50% inhibition were calculated at clinical plasma drug exposures in immune cells. The translation of these measures was evaluated in ex vivo-stimulated assays in phase 1 healthy volunteers.
RESULTS
JAKinib potencies depended on cytokine stimulus, pSTAT readout and cell type. JAK1-dependent pathways (interferon (IFN)α/pSTAT5, interleukin (IL)-6/pSTAT1) were among the most potently inhibited by all JAKinibs in healthy and RA blood, with filgotinib exhibiting the greatest selectivity for JAK1 pathways. Filgotinib (200 mg once daily) had calculated average daily target inhibition for IFNα/pSTAT5 and IL-6/pSTAT1 that was equivalent to tofacitinib (5 mg two times per day), upadacitinib (15 mg once daily) and baricitinib (4 mg once daily), with the least average daily inhibition for the JAK2-dependent and JAK3-dependent pathways including IL-2, IL-15, IL-4 (JAK1/JAK3), IFNγ (JAK1/JAK2), granulocyte colony stimulating factor, IL-12, IL-23 (JAK2/tyrosine kinase 2) and granulocyte-macrophage colony-stimulating factor (JAK2/JAK2). Ex vivo pharmacodynamic data from phase 1 healthy volunteers clinically confirmed JAK1 selectivity of filgotinib.
CONCLUSION
Filgotinib inhibited JAK1-mediated signalling similarly to other JAKinibs, but with less inhibition of JAK2-dependent and JAK3-dependent pathways, providing a mechanistic rationale for its apparently differentiated efficacy:safety profile.
目的
Janus 激酶抑制剂(JAKinibs)在类风湿关节炎(RA)中具有疗效,但不良事件的报告率存在差异,这可能与不同的 JAK 家族成员选择性有关。本文比较了 filgotinib 与 baricitinib、tofacitinib 和 upadacitinib,以阐明其临床疗效和安全性的药理学基础。
方法
通过流式细胞术,在外周血单个核细胞和健康供体及 RA 患者的全血中,检测细胞因子刺激不同 JAK/STAT 通路后信号转导和转录激活因子磷酸化(pSTAT)的体外 JAKinib 抑制情况。在免疫细胞的临床血浆药物暴露水平下,计算平均每日 pSTAT 和超过 50%抑制的时间。在 1 期健康志愿者的体外刺激试验中评估这些措施的转化。
结果
JAKinib 的效力取决于细胞因子刺激、pSTAT 读数和细胞类型。JAK1 依赖性途径(干扰素(IFN)α/pSTAT5、白细胞介素(IL)-6/pSTAT1)在健康人和 RA 血液中被所有 JAKinib 强烈抑制,其中 filgotinib 对 JAK1 途径具有最大的选择性。Filgotinib(每日一次 200mg)对 IFNα/pSTAT5 和 IL-6/pSTAT1 的平均每日靶抑制作用与 tofacitinib(每日两次 5mg)、upadacitinib(每日一次 15mg)和 baricitinib(每日一次 4mg)相当,对 JAK2 依赖性和 JAK3 依赖性途径(包括 IL-2、IL-15、IL-4(JAK1/JAK3)、IFNγ(JAK1/JAK2)、粒细胞集落刺激因子、IL-12、IL-23(JAK2/酪氨酸激酶 2)和粒细胞-巨噬细胞集落刺激因子(JAK2/JAK2)的平均每日抑制作用最小。来自 1 期健康志愿者的体外药效学数据从临床角度证实了 filgotinib 的 JAK1 选择性。
结论
Filgotinib 抑制 JAK1 介导的信号传递与其他 JAKinibs相似,但对 JAK2 依赖性和 JAK3 依赖性途径的抑制作用较小,为其明显不同的疗效/安全性特征提供了机制上的依据。
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