A Population Pharmacokinetic Model of Tocilizumab in Kidney Transplant Patients Treated for Chronic Active Antibody-Mediated Rejection: Comparison of Plasma Exposure Between Intravenous and Subcutaneous Administration Schemes.

IF 5.4 2区 医学 Q1 IMMUNOLOGY
BioDrugs Pub Date : 2024-09-01 Epub Date: 2024-08-15 DOI:10.1007/s40259-024-00676-z
Capucine Arrivé, Caroline Bazzoli, Thomas Jouve, Johan Noble, Lionel Rostaing, Françoise Stanke-Labesque, Zoubir Djerada
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引用次数: 0

Abstract

Background: Tocilizumab prevents the clinical worsening of chronic active antibody-mediated rejection (CAAMR) in kidney transplant recipients. Following a global shortage of the intravenous pharmaceutical form in 2022, patients were switched from monthly intravenous administration of 8 mg/kg to weekly subcutaneous injection of 162 mg, raising the question of bioequivalence between these schemes of administration.

Aims: We aimed to compare the areas under the curve (AUC) of tocilizumab in virtual simulations of populations treated with the two administration schemes and to identify the covariates that could contribute to pharmacokinetic variability of tocilizumab in kidney transplant patients with CAAMR who received tocilizumab as salvage treatment.

Methods: This retrospective monocentric study included 43 kidney transplant patients (202 tocilizumab concentrations) with CAAMR treated with intravenous or subcutaneous tocilizumab between December 2020 and January 2023. We developed a population pharmacokinetic model using nonlinear mixed effects modeling and identified the covariates that could contribute to tocilizumab AUC variability. Monte Carlo simulations were then performed to assess the subcutaneous and intravenous tocilizumab AUC for 0-28 days (M1), 56-84 days (M3), 140-168 days (M6), and 308-336 days (M12). Bioequivalence was defined by SC/IV AUC geometric mean ratios (GMRs) between 0.80 and 1.25.

Results: A two-compartment model with parallel linear and nonlinear elimination best described the concentration-time data. Significant covariates for tocilizumab clearance were body weight, urinary albumin-to-creatinine ratio (ACR), and inflammation status [C-reactive protein (CRP) ≥ 5 mg/L]. The GMR values and their 90% confidence intervals at M3, M6, and M12 were within the 0.8-1.25 margin for equivalence. Conversely, the 90% prediction intervals of the GMR were much wider than the 90% confidence intervals and did not fall within 0.8 and 1.25.

Conclusions: From month 3 of treatment, the subcutaneous and intravenous tocilizumab administration schemes provided average bioequivalent pharmacokinetic exposure at the population level but not at the individual level. Body weight, inflammation, ACR, and administration scheme should be considered to personalize the dose of tocilizumab for patients with CAAMR. Further studies are required to determine the target of tocilizumab exposure in kidney transplant patients with CAAMR.

Abstract Image

治疗慢性活动性抗体介导的排斥反应的肾移植患者中托珠单抗的群体药代动力学模型:静脉注射与皮下注射血浆暴露量的比较
背景托西珠单抗可预防肾移植受者慢性活动性抗体介导的排斥反应(CAAMR)的临床恶化。2022 年静脉注射剂型出现全球性短缺后,患者从每月静脉注射 8 毫克/千克改为每周皮下注射 162 毫克,这就提出了这两种给药方案之间的生物等效性问题。目的:我们旨在通过虚拟模拟两种给药方案的治疗人群,比较托珠单抗的曲线下面积(AUC),并确定在接受托珠单抗作为挽救性治疗的 CAAMR 肾移植患者中,可能导致托珠单抗药代动力学变异的协变量:这项回顾性单中心研究纳入了2020年12月至2023年1月期间接受静脉或皮下托珠单抗治疗的43例CAAMR肾移植患者(202个托珠单抗浓度)。我们使用非线性混合效应模型建立了一个群体药代动力学模型,并确定了可能导致西利珠单抗 AUC 变异的协变量。然后进行了蒙特卡罗模拟,以评估 0-28 天(M1)、56-84 天(M3)、140-168 天(M6)和 308-336 天(M12)的皮下和静脉注射托西珠单抗 AUC。生物等效性的定义是SC/IV AUC几何平均比(GMR)在0.80和1.25之间:平行线性和非线性消除的两室模型最能描述浓度-时间数据。体重、尿白蛋白-肌酐比值(ACR)和炎症状态[C反应蛋白(CRP)≥ 5 mg/L]是影响托西珠单抗清除率的重要协变量。M3、M6 和 M12 的 GMR 值及其 90% 置信区间在 0.8-1.25 的等效范围内。相反,GMR 的 90% 预测区间比 90% 置信区间宽得多,不在 0.8 和 1.25 的范围内:从治疗的第3个月开始,皮下注射和静脉注射托西珠单抗的给药方案在群体水平上提供了平均的生物等效药代动力学暴露,但在个体水平上并不等效。在为 CAAMR 患者制定个性化的托珠单抗剂量时,应考虑体重、炎症、ACR 和给药方案。需要进一步研究确定 CAAMR 肾移植患者的托珠单抗暴露目标。
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来源期刊
BioDrugs
BioDrugs 医学-免疫学
CiteScore
12.60
自引率
2.90%
发文量
50
审稿时长
>12 weeks
期刊介绍: An essential resource for R&D professionals and clinicians with an interest in biologic therapies. BioDrugs covers the development and therapeutic application of biotechnology-based pharmaceuticals and diagnostic products for the treatment of human disease. BioDrugs offers a range of additional enhanced features designed to increase the visibility, readership and educational value of the journal’s content. Each article is accompanied by a Key Points summary, giving a time-efficient overview of the content to a wide readership. Articles may be accompanied by plain language summaries to assist patients, caregivers and others in understanding important medical advances. The journal also provides the option to include various other types of enhanced features including slide sets, videos and animations. All enhanced features are peer reviewed to the same high standard as the article itself. Peer review is conducted using Editorial Manager®, supported by a database of international experts. This database is shared with other Adis journals.
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