A Phase 1b PK/PD Study to Demonstrate Antigen Elimination with RLYB212, a Monoclonal Anti-HPA-1a Antibody for FNAIT Prevention.

IF 5 2区 医学 Q1 HEMATOLOGY Thrombosis and haemostasis Pub Date : 2024-09-12 DOI:10.1055/a-2398-9344
Christof Geisen, Erika Fleck, Stephan Martin Gastón Schäfer, Carmen Walter, Susanne Braeuninger, Jens Søndergaard Jensen, Douglas Sheridan, Kiran Patki, Róisín Armstrong, Bjørn Skogen, Frank Behrens, Erhard Seifried, Jens Kjeldsen-Kragh, Mette Kjær, Michaela Köhm
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Abstract

Background:  Fetal and neonatal alloimmune thrombocytopenia (FNAIT) is a rare bleeding disorder of the fetus/newborn caused by development of maternal alloantibodies against fetal human platelet antigens (HPAs), predominantly HPA-1a. Currently there are no treatments available to prevent maternal alloimmunization to HPAs or FNAIT.

Methods:  This proof-of-concept study (EudraCT Number: 2021-005380-49) was designed to assess the ability of subcutaneous (SC) RLYB212, a monoclonal anti-HPA-1a antibody, to eliminate HPA-1a-positive platelets in an antigen challenge model of a 30 mL fetal-maternal hemorrhage. Subjects were randomized to receive a single SC dose of RLYB212 or placebo on day 1 in a single-blinded manner, followed by transfusion of 10 × 109 HPA-1a-positive platelets on day 8.

Results:  Four subjects received 0.09 mg SC RLYB212, five received 0.29 mg SC RLYB212, and two received placebo. RLYB212 achieved rapid elimination of HPA-1a-positive platelets in a concentration-dependent manner, with concentrations as low as 3.57 ng/mL meeting the prespecified proof-of-concept criterion of ≥90% reduction in platelet elimination half-life versus placebo. Following HPA-1a-positive platelet transfusion, a rapid decline was observed in the concentration of RLYB212 over a period of 2 to 24 hours, corresponding to the time needed for RLYB212 to bind to ∼10% of HPA-1a on cell surfaces. RLYB212 was well tolerated with no reports of drug-related adverse events.

Conclusion:  The data from this study are consistent with preclinical efficacy data and support the potential use of RLYB212 as a prophylactic treatment for FNAIT that prevents maternal HPA-1a alloimmunization during at-risk pregnancies.

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用于预防 FNAIT 的单克隆抗 HPA-1a 抗体 RLYB212 的 1b 期 PK/PD 研究证明了抗原消除作用。
背景:胎儿和新生儿同种免疫血小板减少症(FNAIT)是一种罕见的胎儿/新生儿出血性疾病,由母体产生的针对胎儿人类血小板抗原(HPAs)(主要是HPA-1a)的同种抗体引起。目前还没有预防母体对 HPAs 或 FNAIT 产生同种免疫的治疗方法:这项概念验证研究(EudraCT 编号:2021-005380-49)旨在评估单克隆抗 HPA-1a 抗体皮下 (SC) RLYB212 在 30 mL 胎儿-产妇出血抗原挑战模型中消除 HPA-1a 阳性血小板的能力。受试者在第1天以单盲方式随机接受单剂量RLYB212或安慰剂,然后在第8天输注10 × 10^9 HPA-1a阳性血小板:4名受试者接受了0.09毫克的RLYB212皮下注射,5名受试者接受了0.29毫克的RLYB212皮下注射,2名受试者接受了安慰剂。RLYB212 能以浓度依赖性方式快速消除 HPA-1a 阳性血小板,低至 3.57 纳克/毫升的浓度符合预设的概念验证标准,即与安慰剂相比,血小板消除半衰期缩短≥90%。输注 HPA-1a 阳性血小板后,RLYB212 的浓度在 2 到 24 小时内迅速下降,这与 RLYB212 与细胞表面约 10% 的 HPA-1a 结合所需的时间相符。RLYB212 的耐受性良好,没有与药物相关的不良反应报告:本研究的数据与临床前疗效数据一致,支持将 RLYB212 用作 FNAIT 的预防性治疗,以防止高危妊娠期间母体的 HPA-1a 同种免疫。
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来源期刊
Thrombosis and haemostasis
Thrombosis and haemostasis 医学-外周血管病
CiteScore
11.90
自引率
9.00%
发文量
140
审稿时长
1 months
期刊介绍: Thrombosis and Haemostasis publishes reports on basic, translational and clinical research dedicated to novel results and highest quality in any area of thrombosis and haemostasis, vascular biology and medicine, inflammation and infection, platelet and leukocyte biology, from genetic, molecular & cellular studies, diagnostic, therapeutic & preventative studies to high-level translational and clinical research. The journal provides position and guideline papers, state-of-the-art papers, expert analysis and commentaries, and dedicated theme issues covering recent developments and key topics in the field.
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