Felten Renaud, Scher Florence, Sagez Flora, Chasset François, Arnaud Laurent
Rheumatology Department, University Hospital of Strasbourg, Université de Strasbourg, Strasbourg, F-67000, France.
National Reference Centre for Rare Systemic and Autoimmune Diseases East South-West (RESO), Strasbourg, France.
Drug Des Devel Ther. 2019 May 8;13:1535-1543. doi: 10.2147/DDDT.S170969. eCollection 2019.
Previous reports have described the appearance of systemic lupus erythematosus (SLE) cases following interferon-α (IFN-α) therapy, IFN-regulated gene expression is significantly increased in SLE, and an association between SLE and gene variants belonging to IFN downstream pathways has been shown. Based on this, targeting of IFN and of their signaling pathways has appeared to be interesting developments within the field of SLE therapy. Different specific type I IFN antagonists have been studied in clinical trials and some of those have already reached Phase III. A potential approach would be to target IFN receptors rather than IFN themselves. Anifrolumab (previously MEDI-546) is a fully human monoclonal antibody (Ab) that binds to subunit 1 of the type I IFN receptor (IFNAR1), blocking the action of different type I IFNs (IFN-α, IFN-β and IFN-ω). This drug has been assessed in 11 clinical studies: 9 in SLE, 1 in systemic sclerosis and 1 in rheumatoid arthritis. In SLE, clinical development reached Phase I for 1 study and Phases II and III for 5 and 3 trials, respectively. The Phase IIb, randomized control trial (RCT), double-blind, placebo-controlled study of adults with moderate-to-severe SLE (MUSE trial) showed positive results on the composite primary endpoint SRI-4. Greater efficacy was seen in patients with high baseline IFN gene signature compared with those with low baseline IFN gene signature. Anifrolumab also demonstrated promising results on cutaneous and arthritic manifestations, especially among patients with a high IFN gene signature. The pivotal Treatment of Uncontrolled Lupus via the Interferon IFN Pathway (TULIP 1 and 2 studies are now completed. In August 2018, the promoter announced that the TULIP 1 Phase III trial did not reach its primary endpoint. The release of the completed but not yet published Phase II studies and of the TULIP pivotal trials results will further inform us on the actual therapeutic potential of anifrolumab.
既往报告描述了干扰素-α(IFN-α)治疗后出现系统性红斑狼疮(SLE)病例的情况,SLE中IFN调节的基因表达显著增加,并且已显示SLE与IFN下游通路的基因变异之间存在关联。基于此,靶向IFN及其信号通路似乎已成为SLE治疗领域中有趣的进展。不同的特异性I型IFN拮抗剂已在临床试验中进行了研究,其中一些已进入III期。一种潜在的方法可能是靶向IFN受体而非IFN本身。阿尼鲁单抗(以前称为MEDI-546)是一种完全人源化单克隆抗体(Ab),可与I型IFN受体(IFNAR1)的亚基1结合,阻断不同I型IFN(IFN-α、IFN-β和IFN-ω)的作用。该药物已在11项临床研究中进行了评估:9项针对SLE,1项针对系统性硬化症,1项针对类风湿性关节炎。在SLE中,1项研究进入了I期临床开发,5项和3项试验分别进入了II期和III期。针对中重度SLE成人患者的IIb期随机对照试验(RCT)、双盲、安慰剂对照研究(MUSE试验)在复合主要终点SRI-4上显示出阳性结果。与基线IFN基因特征低的患者相比,基线IFN基因特征高的患者疗效更佳。阿尼鲁单抗在皮肤和关节表现方面也显示出有前景的结果,尤其是在IFN基因特征高的患者中。关键的通过干扰素IFN通路治疗难治性狼疮(TULIP 1和2研究)现已完成。2018年8月,申办方宣布TULIP 1 III期试验未达到其主要终点。已完成但尚未发表的II期研究以及TULIP关键试验结果的公布将进一步让我们了解阿尼鲁单抗的实际治疗潜力。
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