评估 Tour006 在患有慢性肾脏病和 Hs-CRP 升高的参与者中的应用:Tranquility 2 期研究的原理和设计

IF 4.3 Q1 CARDIAC & CARDIOVASCULAR SYSTEMS American journal of preventive cardiology Pub Date : 2024-09-01 DOI:10.1016/j.ajpc.2024.100778
Emil DeGoma MD
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引用次数: 0

摘要

治疗领域药物疗法背景尽管改变了生活方式并进行了强化药物治疗(包括抗血小板药物、降压治疗和降低低密度脂蛋白药物),但动脉粥样硬化性心血管疾病(ASCVD)亚群患者发生重大不良心血管和肢体事件的风险仍然很高。来自人类基因研究、前瞻性队列研究、机理研究以及卡纳金单抗和秋水仙碱心血管病结果试验的综合证据都支持抑制 IL-6 通路的治疗潜力,它可以降低 ASCVD 风险,而不受传统风险因素的影响。TOUR006 是一种针对 IL-6 细胞因子的全人源高亲和性单克隆抗体。在之前的1/2期研究中,类风湿性关节炎、克罗恩病和系统性红斑狼疮等高度炎症性自身免疫疾病患者服用TOUR006后,C反应蛋白(CRP)迅速而持久地下降,CRP是IL-6活性的关键下游药效学(PD)生物标志物,由高灵敏度(hs)测定法评估。根据这些数据建立的药代动力学(PK)/药效学(PD)模型,在虚拟患者中进行的模拟显示,每月和每季度服用 TOUR006 均能显著降低 hs-CRP。这项2期研究的目的是鉴定TOUR006对慢性肾病(CKD)和hs-CRP升高患者的降低hs-CRP效果、安全性、耐受性和PK。TRANQUILITY是一项2期、随机、双盲、安慰剂对照、多中心、美国试验,共招募了约120名CKD 3期或4期、hs-CRP≥2和15 mg/L的患者。参与者将按 CKD 分期进行分层,并随机接受皮下注射 TOUR006 50 毫克(每季度一次)、25 毫克(每季度一次)、15 毫克(每月一次)或安慰剂(图)。主要PD终点是hs-CRP的变化;其他生物标志物包括IL-6、脂蛋白(a)、氧化低密度脂蛋白和纤维蛋白原。结论TRANQUILITY是一项正在进行的试验,预计将于2025年5月完成主要试验,它将评估TOUR006的安全性、耐受性、PK和降低hs-CRP的效果,并为未来在高风险患者中开展的心血管3期研究提供剂量方案和设计依据。
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EVALUATING TOUR006 IN PARTICIPANTS WITH CHRONIC KIDNEY DISEASE AND ELEVATED HS-CRP: RATIONALE AND DESIGN OF THE TRANQUILITY PHASE 2 STUDY

Therapeutic Area

Pharmacologic Therapy

Background

Subgroups of patients with atherosclerotic cardiovascular disease (ASCVD) remain at very high risk of major adverse cardiovascular and limb events despite lifestyle modification and intensive pharmacological management including antiplatelet drugs, antihypertensive therapy, and LDL-lowering medications. Converging evidence from human genetic studies, prospective cohort studies, and mechanistic studies as well as results of canakinumab and colchicine cardiovascular outcome trials support the therapeutic potential of IL-6 pathway inhibition to lower the risk of ASCVD independent of traditional risk factors. TOUR006 is a fully human, high-affinity monoclonal antibody against the IL-6 cytokine. In prior Phase 1/2 studies, TOUR006 administered to patients with high-grade inflammatory autoimmune diseases such as rheumatoid arthritis, Crohn's disease, and systemic lupus erythematosus achieved rapid and durable reductions in C-reactive protein (CRP), the key downstream pharmacodynamic (PD) biomarker of IL-6 activity, as assessed by the high-sensitivity (hs) assay. A pharmacokinetic (PK)/PD model was developed from these data, and simulations in virtual patients showed significant reductions in hs-CRP with both monthly and quarterly dosing of TOUR006. The objective of this Phase 2 study is to characterize the hs-CRP-lowering effect, safety, tolerability, and PK of TOUR006 in patients with chronic kidney disease (CKD) and elevated hs-CRP. The CKD population was selected for this trial because of the high prevalence of elevated hs-CRP as well as evidence supporting a significant role of IL-6 pathway activation in driving ASCVD risk among patients with CKD.

Methods

TRANQUILITY is a Phase 2, randomized, double-blind, placebo-controlled, multicenter, US-based trial enrolling approximately 120 patients with CKD stage 3 or 4 and hs-CRP≥2 and <15 mg/L. Participants will be stratified by CKD stage and randomized to subcutaneous TOUR006 50 mg quarterly, 25 mg quarterly, 15 mg monthly, or placebo (Figure). The primary PD endpoint is change in hs-CRP; additional biomarkers include IL-6, lipoprotein(a), oxidized LDL, and fibrinogen. Treatment and follow-up periods are 180 days and 185 days, respectively.

Conclusions

TRANQUILITY, an ongoing trial with anticipated primary completion in May 2025, will assess the safety, tolerability, PK, and hs-CRP-lowering effect of TOUR006 and inform the dosing regimen and design of future Phase 3 cardiovascular studies in high-risk patients.
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来源期刊
American journal of preventive cardiology
American journal of preventive cardiology Cardiology and Cardiovascular Medicine
CiteScore
6.60
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审稿时长
76 days
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