Rescue immune tolerance induction with a recombinant factor Fc-fused VIII: prospective ReITIrate study of clinical, humoral and cellular immune responses.

IF 3.4 3区医学 Q2 HEMATOLOGY Therapeutic Advances in Hematology Pub Date : 2024-11-23 eCollection Date: 2024-01-01 DOI:10.1177/20406207241300809

Christoph Königs, Shannon L Meeks, Beatrice Nolan, Anja Schmidt, Malin Löfqvist, Jennifer Dumont, Lisa Leickt, Sushrusha Nayak, Stefan Lethagen

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Abstract

Background: Immune tolerance induction (ITI) is the gold standard for inhibitor eradication to restore the clinical efficacy of factor replacement therapy in haemophilia. However, as ITI often requires frequent administration over extended periods, it can be considered burdensome for patients and healthcare resources. Therefore, there is a need to optimise ITI treatment, particularly in patients who failed previous ITI attempts.

Objectives: The ReITIrate study aimed to prospectively evaluate rescue ITI with efmoroctocog alfa, an extended half-life recombinant FVIII Fc fusion protein (herein rFVIIIFc), within a limited 60-week timeframe in patients with severe haemophilia A and inhibitors who failed previous ITI attempts.

Design: ReITIrate was a phase IV, open-label, single-arm, interventional, multicentre study.

Methods: Primary endpoint was ITI success (negative titre, <0.6 BU/mL; incremental recovery >66%; elimination half-life ⩾7 hours) within 60 weeks. Exploratory immunophenotype analyses were performed to characterise anti-drug antibodies (ADA) and cellular immune responses.

Results: Nine of 16 enrolled subjects completed the ITI period during ReITIrate, of which one subject attained all 3 ITI success criteria after 46 weeks with no relapse. Two subjects achieved partial success (one subject met 2/3 success criteria; one met all criteria, but not simultaneously, with inhibitor recurrence). One additional subject (ITI failure) achieved negative inhibitor titre. Across these four subjects, median (range) time to negative titre was 19 (11-60) weeks. No new safety concerns were identified. IgG4 was the major contributor to the ADA IgG response. Subjects with partial/complete ITI success had fewer IgG subclasses involved than those who failed/withdrew. Immunophenotyping indicated an increase in regulatory T-cells (CD4⁺CD25⁺CD127^low), supporting the ability to perform sensitive blood sampling to identify immune tolerance markers.

Conclusion: This study demonstrates that ITI with rFVIIIFc given within a limited timeframe has potential benefit in a difficult-to-treat inhibitor haemophilia population who failed previous ITI attempts.

Trial registration: NCT03103542.

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用融合 Fc 的重组因子 VIII 诱导免疫耐受：临床、体液和细胞免疫反应的前瞻性 ReITIrate 研究。

背景：免疫耐受诱导（ITI）是根除抑制剂以恢复血友病因子替代疗法临床疗效的黄金标准。然而，由于免疫耐受诱导通常需要在较长时间内频繁用药，因此会给患者和医疗资源造成负担。因此，有必要优化 ITI 治疗，尤其是对之前尝试 ITI 失败的患者：ReITIrate研究旨在前瞻性地评估使用efmoroctocog alfa（一种半衰期延长的重组FVIII Fc融合蛋白，以下简称rFVIIIFc）在有限的60周时间内对既往ITI尝试失败的重度A型血友病患者和抑制剂患者进行抢救性ITI治疗的效果：ReITIrate是一项IV期、开放标签、单臂、介入、多中心研究：主要终点是 60 周内 ITI 成功（滴度阴性，66%；消除半衰期⩾7 小时）。对抗药性抗体（ADA）和细胞免疫反应进行了探索性免疫表型分析：16 名注册受试者中有 9 名在 ReITIrate 期间完成了 ITI 期，其中一名受试者在 46 周后达到了全部 3 项 ITI 成功标准，并且没有复发。两名受试者取得了部分成功（一名受试者达到了 2/3 的成功标准；一名受试者达到了所有标准，但未同时达到，且抑制剂复发）。另有一名受试者（ITI 失败）的抑制剂滴度为阴性。在这四名受试者中，滴度呈阴性的中位时间（范围）为 19（11-60）周。未发现新的安全性问题。IgG4 是导致 ADA IgG 反应的主要因素。与失败/退出的受试者相比，部分/完全 ITI 成功的受试者涉及的 IgG 亚类较少。免疫分型显示调节性 T 细胞（CD4+CD25+CD127-low）增加，这支持了进行敏感的血液采样以确定免疫耐受标记物的能力：这项研究表明，在有限的时间内使用 rFVIIIFc 进行 ITI，对之前 ITI 尝试失败、难以治疗的抑制剂血友病患者有潜在益处：试验注册：NCT03103542。

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

Therapeutic Advances in Hematology HEMATOLOGY-

CiteScore

4.30

自引率

0.00%

发文量

审稿时长

7 weeks

期刊介绍： Therapeutic Advances in Hematology delivers the highest quality peer-reviewed articles, reviews, and scholarly comment on pioneering efforts and innovative studies across all areas of hematology. The journal has a strong clinical and pharmacological focus and is aimed at clinicians and researchers in hematology, providing a forum in print and online for publishing the highest quality articles in this area.