Pharmacokinetics and immunogenicity of eftozanermin alfa in subjects with previously-treated solid tumors or hematologic malignancies: results from a phase 1 first-in-human study.

IF 2.7 4区医学 Q3 ONCOLOGY Cancer Chemotherapy and Pharmacology Pub Date : 2024-04-01 Epub Date: 2023-11-30 DOI:10.1007/s00280-023-04613-9

Carla Biesdorf, Xiaowen Guan, Satya R Siddani, David Hoffman, Nils Boehm, Bruno C Medeiros, Toshihiko Doi, Maja de Jonge, Drew Rasco, Rajeev M Menon, Akshanth R Polepally

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Abstract

Purpose: Eftozanermin alfa is a second-generation tumor necrosis factor-related apoptosis-inducing ligand (TRAIL) receptor agonist that enhances death receptor 4/5 clustering on tumor cells to induce apoptosis. We report the pharmacokinetics and immunogenicity of eftozanermin alfa administered intravenously to 153 adults with previously-treated solid tumors or hematologic malignancies from the first-in-human, open-label, dose-escalation and dose-optimization study.

Methods: Dose escalation evaluated eftozanermin alfa monotherapy 2.5-15 mg/kg on Day 1 or Days 1/8 of a 21-day cycle. Dose optimization evaluated eftozanermin alfa monotherapy or combination therapy with either oral venetoclax 400-800 mg daily (eftozanermin alfa 1.25-7.5 mg/kg Days 1/8/15 of a 21-day cycle) or chemotherapy (eftozanermin alfa 3.75 or 7.5 mg/kg Days 1/8/15/22 of a 28-day cycle and FOLFIRI regimen [leucovorin, 5-fluorouracil, and irinotecan] with/without bevacizumab on Days 1/15 of a 28-day cycle).

Results: Systemic exposures (maximum observed concentration [C_max] and area under the concentration-time curve [AUC]) of eftozanermin alfa were approximately dose-proportional across the entire dose escalation range with minimal to no accumulation in Cycle 3 versus Cycle 1 exposures. Comparable exposures and harmonic mean half-lives (35.1 h [solid tumors], 31.3 h [hematologic malignancies]) were observed between malignancy types. Exposures (dose-normalized C_max and AUC) in Japanese subjects were similar to non-Japanese subjects. Furthermore, eftozanermin alfa/venetoclax combination therapy did not have an impact on the exposures of either agent. Treatment-emergent anti-drug antibodies were observed in 9.4% (13/138) of subjects.

Conclusions: The study results, including a pharmacokinetic profile consistent with weekly dosing and low incidence of immunogenicity, support further investigation of eftozanermin alfa.

Trial registration id: NCT03082209.

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eftozanermin alfa在既往治疗过的实体瘤或血液恶性肿瘤患者中的药代动力学和免疫原性:来自1期首次人体研究的结果

目的:Eftozanermin alfa是第二代肿瘤坏死因子相关凋亡诱导配体(TRAIL)受体激动剂，可增强肿瘤细胞上死亡受体4/5聚集诱导凋亡。我们报告了首次在人体中进行的开放标签、剂量递增和剂量优化研究，对153名既往治疗过实体瘤或血液恶性肿瘤的成年人静脉注射eftozanermin α的药代动力学和免疫原性。方法:在21天周期的第1天或第1/8天，评估eftozanermin α α单药2.5- 15mg /kg的剂量递增。剂量优化评估了eftozanermin alfa单药或联合治疗，每日口服venetoclax 400-800 mg (eftozanermin alfa 1.25-7.5 mg/kg, 21天周期的1/8/15天)或化疗(eftozanermin alfa 3.75或7.5 mg/kg, 28天周期的1/8/15/22天和FOLFIRI方案[亚叶酸钙、5-氟尿嘧啶和伊立替康]，28天周期的1/15天，有/没有贝伐单抗)。结果:eftozanermin α的全身暴露(最大观察浓度[Cmax]和浓度-时间曲线下面积[AUC])在整个剂量递增范围内近似与剂量成正比，在第3周期与第1周期暴露中几乎没有积累。在不同类型的恶性肿瘤中观察到相似的暴露和调和平均半衰期(35.1 h[实体瘤]，31.3 h[血液学恶性肿瘤])。日本受试者的暴露(剂量标准化Cmax和AUC)与非日本受试者相似。此外，eftozanermin /venetoclax联合治疗对任何一种药物的暴露都没有影响。9.4%(13/138)的受试者出现治疗后出现的抗药物抗体。结论:研究结果，包括与每周给药一致的药代动力学特征和低免疫原性发生率，支持对eftozanermin α fa的进一步研究。试验注册id: NCT03082209。

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

Cancer Chemotherapy and Pharmacology 医学-药学

CiteScore

6.10

自引率

3.30%

发文量

116

审稿时长

2.5 months

期刊介绍： Addressing a wide range of pharmacologic and oncologic concerns on both experimental and clinical levels, Cancer Chemotherapy and Pharmacology is an eminent journal in the field. The primary focus in this rapid publication medium is on new anticancer agents, their experimental screening, preclinical toxicology and pharmacology, single and combined drug administration modalities, and clinical phase I, II and III trials. It is essential reading for pharmacologists and oncologists giving results recorded in the following areas: clinical toxicology, pharmacokinetics, pharmacodynamics, drug interactions, and indications for chemotherapy in cancer treatment strategy.