Safety, pharmacokinetics, and pharmacodynamics of efzimfotase alfa, a second-generation enzyme replacement therapy: phase 1, dose-escalation study in adults with hypophosphatasia.

IF 5.1 1区 医学 Q1 ENDOCRINOLOGY & METABOLISM
Kathryn M Dahir, Amy Shannon, Derek Dunn, Walter Voegtli, Qunming Dong, Jawad Hasan, Rajendra Pradhan, Ryan Pelto, Wei-Jian Pan
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引用次数: 0

Abstract

Hypophosphatasia (HPP) is a rare, inherited metabolic disease caused by deficient activity of tissue-nonspecific alkaline phosphatase (TNSALP). Efzimfotase alfa (ALXN1850) is a second-generation TNSALP enzyme replacement therapy in development for HPP. This first-in-human open-label, dose-escalating phase 1 trial evaluated efzimfotase alfa safety, tolerability, pharmacokinetics, pharmacodynamics, and immunogenicity. Fifteen adults (5/cohort) with HPP received efzimfotase alfa in doses of 15 mg (cohort 1), 45 mg (cohort 2), or 90 mg (cohort 3) as one intravenous (i.v.) dose followed by 3 weekly subcutaneous (s.c.) doses. The primary objective was to assess safety and tolerability. Secondary objectives included pharmacokinetics, pharmacodynamics of ALP substrates known to be biomarkers of disease (inorganic pyrophosphate [PPi] and pyridoxal 5'-phosphate [PLP]) and immunogenicity. Treatment-emergent adverse events (TEAEs) occurred in 12 (80%) participants. Eight (53%) participants had injection site reactions (ISRs), observed after 10 of 41 (24%) s.c. injections. Most ISR TEAEs were mild and resolved within 1-2 d. Peak and total exposures of efzimfotase alfa increased in a greater-than-dose proportional manner over the range of 15-90 mg after i.v. and s.c. dosing. The arithmetic mean elimination half-life was approximately 6 d; absolute bioavailability was 28.6%-36.8% over the s.c. dose range of 15-90 mg. Dose-dependent reductions in plasma concentrations of PPi and PLP relative to baseline reached nadir in the first week after i.v. dosing and were sustained for 3-4 wk after the last s.c. dose. Four (27%) participants tested positive for antidrug antibodies (ADAs), 3 of whom were ADA positive before the first dose of efzimfotase alfa. ADAs had no apparent effect on efzimfotase alfa pharmacokinetics/pharmacodynamics. No participants had neutralizing antibodies. Efzimfotase alfa demonstrated acceptable safety, tolerability, and pharmacokinetic profiles and was associated with sustained reductions in biomarkers of disease in adults with HPP, supporting further evaluation in adult and pediatric patients. Registration: ClinicalTrials.gov NCT04980248 (https://clinicaltrials.gov/study/NCT04980248).

第二代酶替代疗法 Efzimfotase Alfa 的安全性、药代动力学和药效学:针对成人低磷酸盐血症患者的第一阶段剂量递增研究。
低磷酸盐血症(HPP)是一种罕见的遗传性代谢疾病,由组织非特异性碱性磷酸酶(TNSALP)活性不足引起。Efzimfotase alfa(ALXN1850)是一种正在开发的第二代 TNSALP 酶替代疗法,用于治疗 HPP。这项首次人体开放标签、剂量递增的 1 期试验评估了 efzimfotase alfa 的安全性、耐受性、药代动力学、药效学和免疫原性。15名成人HPP患者(每组5人)分别接受了15毫克(第一组)、45毫克(第二组)或90毫克(第三组)的依非齐莫特酶α静脉注射,之后每周3次静脉注射。首要目标是评估安全性和耐受性。次要目标包括药代动力学、作为疾病生物标志物的ALP底物(无机焦磷酸[PPi]和5'-磷酸吡哆醛[PLP])的药效学和免疫原性。12名参与者(80%)发生了治疗突发不良事件(TEAEs)。8名参与者(53%)出现注射部位反应(ISR),在41例静脉注射中的10例(24%)后观察到。大多数 ISR TEAEs 都很轻微,并在 1-2 天内缓解。在静脉注射和皮下注射 15-90 毫克后,依夫唑莫特酶 alfa 的峰值和总暴露量会以高于剂量比例的方式增加。算术平均消除 t½ 约为 6 天;在 15-90 毫克的静脉注射剂量范围内,绝对生物利用度为 28.6% 至 36.8%。相对于基线,PPi 和 PLP 的血浆浓度随剂量降低,在静脉注射后第一周达到最低点,并在最后一次静脉注射后持续 3-4 周。四名参与者(27%)的抗药抗体(ADA)检测呈阳性,其中三人在首次服用埃夫齐莫特酶α前ADA呈阳性。ADA对依夫莫特酶α的药代动力学/药效学没有明显影响。没有参与者的中和抗体呈阳性。Efzimfotase alfa具有可接受的安全性、耐受性和药代动力学特征,并能持续降低成人HPP患者的疾病生物标志物,支持在成人和儿童患者中进行进一步评估:注册:NCT04980248。
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
Journal of Bone and Mineral Research
Journal of Bone and Mineral Research 医学-内分泌学与代谢
CiteScore
11.30
自引率
6.50%
发文量
257
审稿时长
2 months
期刊介绍: The Journal of Bone and Mineral Research (JBMR) publishes highly impactful original manuscripts, reviews, and special articles on basic, translational and clinical investigations relevant to the musculoskeletal system and mineral metabolism. Specifically, the journal is interested in original research on the biology and physiology of skeletal tissues, interdisciplinary research spanning the musculoskeletal and other systems, including but not limited to immunology, hematology, energy metabolism, cancer biology, and neurology, and systems biology topics using large scale “-omics” approaches. The journal welcomes clinical research on the pathophysiology, treatment and prevention of osteoporosis and fractures, as well as sarcopenia, disorders of bone and mineral metabolism, and rare or genetically determined bone diseases.
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