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Selective JAK inhibitors in development for rheumatoid arthritis

机译:类风湿关节炎研究中的选择性JAK抑制剂

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Introduction: The JAK kinases are a family of four tyrosine receptor kinases that play a pivotal role in cytokine receptor signalling pathways via their interaction with signal transducers and activators of transcription proteins. Selective inhibitors of JAK kinases are viewed as of considerable potential as disease-modifying anti-inflammatory drugs for the treatment of rheumatoid arthritis.Areas covered: This article provides a review of the clinical development and available clinical results for those JAK inhibitors currently under investigation. Phase II data for four JAK inhibitors (baricitinib, decernotinib, filgotinib and INCB-039110) are contrasted with that reported for the recently approved JAK inhibitor tofacitinib. The preclinical data on these, in addition to peficitinib, ABT-494, INCB-047986 and AC-410 are also discussed, as are some of the inhibitors in preclinical development.Expert opinion: JAK inhibitors are effective in the treatment of rheumatoid arthritis as evidenced by several inhibitors enabling the majority of treated patients to achieve ACR20 responses, with baricitinib and INCB-039110 both effective when administered once daily. JAK inhibitors differ in isoform specificity profiles, with good efficacy achievable by selective inhibition of either JAK1 (filgotinib or INCB-039110) or JAK3 (decernotinib). It remains to be seen what selectivity provides the optimal side-effect profile and to what extent inhibition of JAK2 should be avoided.
机译:简介:JAK激酶是四个酪氨酸受体激酶家族,通过与信号转导子和转录蛋白激活剂相互作用,在细胞因子受体信号通路中发挥关键作用。 JAK激酶的选择性抑制剂被认为是治疗类风湿性关节炎的疾病改良抗炎药,具有很大的潜力。涵盖范围:本文概述了目前正在研究的那些JAK抑制剂的临床发展和可获得的临床结果。四种JAK抑制剂(baricitinib,decernotinib,filgotinib和INCB-039110)的II期数据与最近批准的JAK抑制剂tofacitinib的报道相对照。除了培非替尼,ABT-494,INC-047986和AC-410以外,还讨论了这些药物的临床前数据,以及一些临床前开发抑制剂。专家意见:JAK抑制剂可有效治疗类风湿关节炎有证据表明,几种抑制剂使大多数接受治疗的患者都能实现ACR20反应,而Baricitinib和INCB-039110每天给药一次均有效。 JAK抑制剂的同工型特异性谱不同,可以通过选择性抑制JAK1(filgotinib或INCB-039110)或JAK3(decernotinib)获得良好的疗效。尚有待观察的是哪种选择性可提供最佳的副作用,以及应在多大程度上避免抑制JAK2。

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