Pharmacokinetic and Pharmacodynamic Relationship of Blinatumomab in Patients with Non-Hodgkin Lymphoma.

IF 3.2 Q2 Pharmacology, Toxicology and Pharmaceutics Current clinical pharmacology Pub Date : 2018-01-01 DOI:10.2174/1574884713666180518102514
Youssef Hijazi, Matthias Klinger, Andrea Kratzer, Benjamin Wu, Patrick A Baeuerle, Peter Kufer, Andreas Wolf, Dirk Nagorsen, Min Zhu
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引用次数: 17

Abstract

Background: Blinatumomab is a bispecific T-cell engager (BiTE®) antibody construct targeting CD3ε on T cells and CD19 on B cells. We describe the relationship between pharmacokinetics (PK) of blinatumomab and pharmacodynamic (PD) changes in peripheral lymphocytes, serum cytokines, and tumor size in patients with non-Hodgkin lymphoma (NHL).

Methods: In a phase 1 study, 76 patients with relapsed/refractory NHL received blinatumomab by continuous intravenous infusion at various doses (0.5 to 90 µg/m2/day). PD changes were analyzed with respect to dose, blinatumomab concentration at steady state (Css), and cumulative area under the concentration-versus-time curve (AUCcum).

Results: B-cell depletion occurred within 48 hours at doses ≥5 µg/m2/day, followed first-order kinetics, and was blinatumomab exposure-dependent. Change in tumor size depended on systemic blinatumomab exposure and treatment duration and could be fitted to an Emax model, which predicted a 50% reduction in tumor size at AUCcum of ≥1,340 h×µg/L and Css of ≥1,830 pg/mL, corresponding to a blinatumomab dose of 47 µg/m2/day for 28 days. The magnitude of transient cytokine elevation, observed within 1-2 days of infusion start, was dose-dependent, with less pronounced elevation at low starting doses.

Conclusion: B-lymphocyte depletion following blinatumomab infusion was exposure-dependent. Transient cytokine elevation increased with dose; it was less pronounced at low starting doses. Tumor response was a function of exposure, suggesting utility for the PK/PD relationship in dose selection for future studies, including NHL and other malignant settings.

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布林纳单抗在非霍奇金淋巴瘤患者中的药动学和药效学关系。
背景:Blinatumomab是一种双特异性T细胞接合器(BiTE®)抗体,靶向T细胞上的CD3ε和B细胞上的CD19。我们描述了blinatumomab的药代动力学(PK)与非霍奇金淋巴瘤(NHL)患者外周血淋巴细胞、血清细胞因子和肿瘤大小的药效学(PD)变化之间的关系。方法:在一项1期研究中,76例复发/难治性NHL患者连续静脉输注不同剂量的blinatumumab(0.5至90µg/m2/天)。PD变化与剂量、稳态blinatumomab浓度(Css)和浓度-时间曲线下的累积面积(aucum)有关。结果:在剂量≥5µg/m2/天的情况下,b细胞在48小时内发生损耗,遵循一级动力学,并且与blinatumumab暴露相关。肿瘤大小的变化取决于布利纳单抗的全身暴露和治疗时间,并可拟合Emax模型,该模型预测肿瘤大小在aucum≥1,340 hxµg/L时减少50%,Css≥1,830 pg/mL,对应于布利纳单抗剂量为47µg/m2/天,持续28天。在输注开始后1-2天内观察到的短暂细胞因子升高的幅度是剂量依赖性的,在低起始剂量时升高不太明显。结论:布利纳单抗输注后的b淋巴细胞耗竭是暴露依赖性的。细胞因子瞬时升高随剂量增加而增加;在起始剂量较低时,效果不那么明显。肿瘤反应是暴露的函数,这表明在未来的研究中,包括NHL和其他恶性情况下,PK/PD关系在剂量选择中的效用。
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Current clinical pharmacology
Current clinical pharmacology PHARMACOLOGY & PHARMACY-
CiteScore
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期刊介绍: Current Clinical Pharmacology publishes frontier reviews on all the latest advances in clinical pharmacology. The journal"s aim is to publish the highest quality review articles in the field. Topics covered include: pharmacokinetics; therapeutic trials; adverse drug reactions; drug interactions; drug metabolism; pharmacoepidemiology; and drug development. The journal is essential reading for all researchers in clinical pharmacology.
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