Pharmacokinetic characterization and exposure-response relationship of crovalimab in the COMMODORE 1, 2 and 3 and COMPOSER trials of patients with paroxysmal nocturnal haemoglobinuria.

IF 3.1 3区医学 Q2 PHARMACOLOGY & PHARMACY

British journal of clinical pharmacology Pub Date : 2025-01-21 DOI:10.1111/bcp.16394

Valérie Cosson, Rong Fu, Austin Kulasekararaj, Jun-Ichi Nishimura, Jens Panse, Alexander Röth, Phillip Scheinberg, Hongyan Tong, Sung-Soo Yoon, Leigh Beveridge, Keisuke Gotanda, Félix Jaminion, Andrea Henrich, Pontus Lundberg, Dayu Shi, Sasha Sreckovic, Yuchen Zhang, Zilu Zhang, Khaled Benkali, Simon Buatois

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引用次数: 0

Abstract

Aims: Crovalimab is a novel C5 inhibitor administered first intravenously and then subcutaneously in patients with paroxysmal nocturnal haemoglobinuria (PNH) naive to complement inhibition or switching from eculizumab or ravulizumab. Crovalimab showed efficacy and safety comparable to eculizumab in the pivotal COMMODORE 2 and supporting studies.

Methods: We characterized crovalimab pharmacokinetics and the relationship between exposure pharmacokinetic parameters and pharmacodynamic biomarkers, efficacy and safety endpoints using pooled data (healthy volunteers [n = 9], naive [n = 210] and switched [n = 211] patients). Pharmacodynamic biomarkers included 50% complement activity and free C5; normalized lactate dehydrogenase was a marker of haemolysis. Adverse events (AEs) of special interest, related serious AEs, related Grade ≥3 AEs and infections were assessed.

Results: There was no clinically relevant difference in crovalimab concentrations between naive and switch patients. Bodyweight had a statistically significant impact on crovalimab clearances and volumes of distribution. Thus, the recommended dosing regimen used weight-based, two-tiered dosing (100 kg cutoff). Age did not have a clinically meaningful impact on crovalimab exposure. In COMMODORE 2, and the supporting COMMODORE 1 and 3 studies, complete terminal complement activity inhibition was achieved immediately at the end of the initial intravenous infusion and sustained throughout the treatment period in ≥97% of patients. Crovalimab concentrations above ≈100 μg/mL achieved complete inhibition of terminal complement activity, resulting in disease control with normalized lactate dehydrogenase ≤1.5 × upper limit of normal (ULN). There was no increased risk of AEs at higher exposure.

Conclusions: These data confirm an effective crovalimab-dosing regimen that achieves complete terminal complement activity inhibition and disease control in patients with PNH.

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克罗伐单抗在发作性夜间血红蛋白尿患者的COMMODORE 1、2、3和COMPOSER试验中的药代动力学特征和暴露-反应关系

目的：Crovalimab是一种新型C5抑制剂，首先静脉注射，然后皮下注射，用于首次补体抑制或从eculizumab或ravulizumab切换的突发性夜间血红蛋白尿（PNH）患者。Crovalimab在关键的COMMODORE 2和支持性研究中显示出与eculizumab相当的疗效和安全性。方法：我们使用汇总数据（健康志愿者[n = 9]，初试[n = 210]和切换[n = 211]患者）表征克罗伐单抗的药代动力学以及暴露药代动力学参数与药效学生物标志物、疗效和安全性终点之间的关系。药效学生物标志物包括50%补体活性和游离C5；乳酸脱氢酶正常是溶血的标志。评估特别关注的不良事件（ae）、相关严重ae、相关≥3级ae和感染。结果：克罗伐单抗浓度在初始和转换患者之间没有临床相关性差异。体重对克罗伐单抗清除率和分布量有统计学上显著的影响。因此，推荐的给药方案采用以体重为基础的两级给药（100公斤的截止剂量）。年龄对克罗伐单抗暴露没有临床意义的影响。在COMMODORE 2和支持性的COMMODORE 1和3研究中，≥97%的患者在初始静脉输注结束时立即实现完全的终末补体活性抑制，并持续整个治疗期。克罗伐单抗浓度≈100 μg/mL以上可完全抑制末端补体活性，使正常乳酸脱氢酶≤1.5倍正常上限（ULN）的疾病得到控制。暴露程度越高，发生不良反应的风险也就越高。结论：这些数据证实了一种有效的crovalimumab给药方案，可以在PNH患者中实现完全的终末补体活性抑制和疾病控制。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

British journal of clinical pharmacology 医学-药学

CiteScore

6.30

自引率

8.80%

发文量

419

审稿时长

1 months

期刊介绍： Published on behalf of the British Pharmacological Society, the British Journal of Clinical Pharmacology features papers and reports on all aspects of drug action in humans: review articles, mini review articles, original papers, commentaries, editorials and letters. The Journal enjoys a wide readership, bridging the gap between the medical profession, clinical research and the pharmaceutical industry. It also publishes research on new methods, new drugs and new approaches to treatment. The Journal is recognised as one of the leading publications in its field. It is online only, publishes open access research through its OnlineOpen programme and is published monthly.