瓦达司他(Vadadustat)每周三次用于透析依赖性慢性肾功能衰竭导致贫血的患者。

IF 9.4 1区 医学 Q1 UROLOGY & NEPHROLOGY
Hakan R Toka, Marializa Bernardo, Steven K Burke, Wenli Luo, Roberto Manllo-Karim, Irfan Ullah, Zhihui Yang, Zhiqun Zhang, James Tumlin
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引用次数: 0

摘要

理由和目的:低氧诱导因子脯氨酰羟化酶抑制剂(HIF-PHIs)可作为一种替代性红细胞生成刺激剂(ESA),用于治疗慢性肾脏病患者的贫血。研究目的:探讨从长效红细胞生成刺激剂(ESA)甲氧基聚乙二醇-表皮生长因子β(MPG-EPO)转为口服缺氧诱导因子脯氨酰羟化酶抑制剂(HIF-PHI)伐杜司他(vadadustat),每周3次与维持MPG-EPO治疗的疗效和安全性:3b期、开放标签、非劣效试验:在美国进行的多中心研究;456 名患有贫血和依赖透析的慢性肾病成人患者:参与者按1:1:1的比例随机接受伐杜司他(起始剂量:600毫克,每周三次)、伐杜司他(起始剂量:900毫克,每周三次)或MPG-EPO治疗,治疗最长52周,治疗结束或提前终止后进行4周安全随访:主要和次要疗效终点分别为主要评估期(第20-26周)和次要评估期(第46-52周)血红蛋白与基线相比的平均变化。非劣效性是指与基线相比血红蛋白平均变化差值的 95% CI 下限高于-0.75 g/dL。其他疗效终点是血红蛋白水平在目标范围内的参与者比例,以及在评估期间因贫血而需要ESA或红细胞输血抢救的参与者比例。输血率较低,各治疗组的输血率相似(伐杜司他组和 MPG-EPO 组分别为 2.7% 和 4.0%)。主要安全性终点为任何治疗突发事件和严重不良事件(AEs):合并伐杜司他组(600 毫克和 900 毫克,每周三次,n=304)后,伐杜司他在主要疗效终点(最小平方平均治疗差异,-0.33;95% CI,-0.53 至 -0.13)和次要疗效终点(-0.33;-0.56 至 -0.09)方面均不劣于 MPG-EPO(n=152)。除伐杜司他 600 毫克组的血红蛋白浓度最初略有下降,但到第 12 周时已趋于稳定外,其他各组的血红蛋白浓度均保持稳定。与伐杜司他联合治疗组(14.2%;7.3%)相比,MPG-EPO 组(主要评估期,27.7%;次要评估期,16.2%)因贫血接受 ESA 治疗的频率更高。各治疗组的任何治疗突发症状和严重治疗突发症状的发生率相似:局限性:与药物相关的AEs归因可能存在误差:每周三次服用伐杜司他对血红蛋白水平的影响不劣于MPG-EPO,且在AEs方面未发现差异。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Vadadustat Three Times Weekly in Patients With Anemia Due to Dialysis-Dependent CKD.

Rationale & objective: Hypoxia-inducible factor prolyl hydroxylase inhibitors (HIF-PHIs) may offer an alternative erythropoiesis-stimulating agents (ESA) for the treatment of anemia in the setting of CKD. To investigate the efficacy and safety of conversion from long-acting erythropoiesis-stimulating agent (ESA) methoxy polyethylene glycol-epoetin beta (MPG-EPO) to the oral hypoxia-inducible factor prolyl hydroxylase inhibitor (HIF-PHI) vadadustat 3-times-weekly versus maintenance on MPG-EPO.

Study design: Phase 3b, open-label, noninferiority trial.

Setting & participants: Multicenter study in United States; 456 patients adults with anemia and dialysis-dependent chronic kidney disease.

Intervention: Participants were randomized 1:1:1 either to vadadustat (starting dose: 600 mg thrice weekly), vadadustat (starting dose: 900 mg thrice weekly), or MPG-EPO, for up to 52 treatment weeks and 4 safety follow-up weeks after the end of treatment or early termination.

Outcomes: Primary and secondary efficacy endpoints were the mean change in hemoglobin from baseline during primary (weeks 20-26) and secondary (weeks 46-52) evaluation periods, respectively. Noninferiority was specified as a lower bound of the 95% CI above -0.75 g/dL for the difference in mean change in hemoglobin from baseline. Other efficacy endpoints were the proportion of participants with hemoglobin levels within the target range and the proportions of participants requiring ESA or red blood cell transfusion rescue for anemia during the evaluation periods. Transfusion rates were low and occurred at similar rates across treatment groups (2.7% and 4.0% in the combined vadadustat and MPG-EPO groups, respectively). Primary safety endpoints were any treatment-emergent and serious adverse events (AEs).

Results: After combining the vadadustat groups (600 mg and 900 mg thrice weekly, n=304), vadadustat was noninferior to MPG-EPO (n=152) for both primary (least squares mean treatment difference, -0.33; 95% CI, -0.53 to -0.13) and secondary efficacy endpoints (-0.33; -0.56 to -0.09). Mean hemoglobin concentrations were stable for all groups, except for an initial slight decline in the vadadustat 600 mg group, which stabilized by week 12. ESA rescue for anemia was more frequent in the MPG-EPO group (primary evaluation period, 27.7%; secondary evaluation period, 16.2%) than in the combined vadadustat (14.2%; 7.3%) groups. The incidences of any treatment-emergent and serious treatment-emergent AEs were similar across treatment groups.

Limitations: Potential errors in attribution of AEs as drug related.

Conclusions: Three-times-weekly vadadustat was noninferior to MPG-EPO on their effect on hemoglobin levels without detectable differences in AEs.

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来源期刊
American Journal of Kidney Diseases
American Journal of Kidney Diseases 医学-泌尿学与肾脏学
CiteScore
20.40
自引率
2.30%
发文量
732
审稿时长
3-8 weeks
期刊介绍: The American Journal of Kidney Diseases (AJKD), the National Kidney Foundation's official journal, is globally recognized for its leadership in clinical nephrology content. Monthly, AJKD publishes original investigations on kidney diseases, hypertension, dialysis therapies, and kidney transplantation. Rigorous peer-review, statistical scrutiny, and a structured format characterize the publication process. Each issue includes case reports unveiling new diseases and potential therapeutic strategies.
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