Riva Natalia, Brstilo Lucas, Sancho-Araiz Aymara, Molina Manuel, Savransky Andrea, Roffé Georgina, Sanz Marianela, Tenembaum Silvia, Katsicas Maria M, Trocóniz Iñaki F, Schaiquevich Paula
Pharmacometrics & Systems Pharmacology Research Unit, Department of Pharmaceutical Sciences, School of Pharmacy and Nutrition, University of Navarra, 31008 Pamplona, Spain.
Unit of Innovative Treatments, Hospital de Pediatría JP Garrahan, Buenos Aires C1245 CABA, Argentina.
Pharmaceutics. 2023 Oct 26;15(11):2534. doi: 10.3390/pharmaceutics15112534.
Limited pharmacotherapy and the failure of conventional treatments in complex pathologies in children lead to increased off-label use of rituximab. We aimed to characterize the time course of CD19+ B lymphocytes (CD19+) under treatment with intravenous rituximab in children with neurologic and autoimmune diseases and to evaluate the impact of covariates (i.e., demographics, diagnosis and substitution between innovator and biosimilar product) on rituximab pharmacodynamics and disease activity.
Pre- and post-drug infusion CD19+ in peripheral blood were prospectively registered. A population pharmacodynamic model describing the time course of CD19+ was developed with NONMEM v7.4. Simulations of three different rituximab regimens were performed to assess the impact on CD19+. Logistic regression analysis was performed to identify predictors of clinical response recorded through disease activity scores.
281 measurements of CD19+ lymphocyte counts obtained from 63 children with neurologic ( = 36) and autoimmune ( = 27) diseases were available. The time course of CD19+ was described with a turn-over model in which the balance between synthesis and degradation rates is disrupted by rituximab, increasing the latter process. The model predicts half-lives (percent coefficient of variation, CV(%)) of rituximab and CD19+ of 11.6 days (17%) and 173.3 days (22%), respectively. No statistically significant effect was found between any of the studied covariates and model parameters ( > 0.05). Simulations of different regimens showed no clinically significant differences in terms of CD19+ repopulation times. A trend towards a lack of clinical response was observed in patients with lower CD19+ repopulation times and higher areas under the CD19+ versus time curve.
Rituximab pharmacodynamics was described in a real-world setting in children suffering from autoimmune and neurologic diseases. Diagnosis, substitution between innovator rituximab and its biosimilars or type of regimen did not affect rituximab-induced depletion of CD19+ nor the clinical response in this cohort of patients. According to this study, rituximab frequency and dosage may be chosen based on clinical convenience or safety reasons without affecting CD19+ repopulation times. Further studies in larger populations are required to confirm these results.
儿童复杂病症的药物治疗有限且传统治疗方法失效,导致利妥昔单抗的超说明书使用增加。我们旨在描述患有神经和自身免疫性疾病的儿童在接受静脉注射利妥昔单抗治疗期间CD19 + B淋巴细胞(CD19 +)的时间进程,并评估协变量(即人口统计学、诊断以及创新药与生物类似药之间的替换)对利妥昔单抗药效学和疾病活动的影响。
前瞻性记录外周血中药物输注前后的CD19 +。使用NONMEM v7.4开发了一个描述CD19 +时间进程的群体药效学模型。进行了三种不同利妥昔单抗方案的模拟,以评估对CD19 +的影响。进行逻辑回归分析,以确定通过疾病活动评分记录的临床反应的预测因素。
从63例患有神经疾病(n = 36)和自身免疫性疾病(n = 27)的儿童中获得了281次CD19 +淋巴细胞计数测量值。CD19 +的时间进程用一个周转模型来描述,其中利妥昔单抗破坏了合成和降解速率之间的平衡,增加了后者的过程。该模型预测利妥昔单抗和CD19 +的半衰期(变异系数百分比,CV(%))分别为11.6天(17%)和173.3天(22%)。在所研究的任何协变量与模型参数之间均未发现统计学上的显著差异(P > 0.05)。不同方案的模拟显示,在CD19 +再填充时间方面没有临床上的显著差异。在CD19 +再填充时间较短且CD19 +随时间变化曲线下面积较大的患者中,观察到缺乏临床反应的趋势。
在患有自身免疫性和神经疾病的儿童的真实世界环境中描述了利妥昔单抗的药效学。诊断、创新型利妥昔单抗与其生物类似药之间的替换或方案类型均未影响利妥昔单抗诱导的CD19 +耗竭或该队列患者的临床反应。根据本研究,可基于临床便利性或安全性原因选择利妥昔单抗的频率和剂量,而不影响CD19 +再填充时间。需要在更大的人群中进行进一步研究以证实这些结果。
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