Division of Hematology, MedStar Georgetown University Hospital, Washington, DC.
Department of Hematology and Stem Cell Transplantation, West German Cancer Center, University Hospital Essen, University of Duisburg-Essen, Essen, Germany.
Blood Adv. 2023 Mar 28;7(6):987-996. doi: 10.1182/bloodadvances.2021006864.
Chronic/refractory immune thrombocytopenia (ITP) is a rare and pathophysiologically heterogeneous disorder with variable responsiveness to available treatments. Sutimlimab, a first-in-class humanized monoclonal anti-C1s IgG4 antibody, selectively inhibits the classical pathway. This phase 1 study (NCT03275454) assessed the safety, efficacy, pharmacokinetics, and pharmacodynamics of biweekly sutimlimab in patients with chronic/refractory ITP with an inadequate response to ≥2 therapies (platelet count ≤ 30 × 109/L). Twelve patients (median age 42 years) received sutimlimab for a median of 20.5 weeks followed by a median 2-week washout period (part A). In part B, 7 of the 12 eligible patients received sutimlimab retreatment for a median of 113 weeks. In part A, the mean (standard deviation) platelet count increased from 25 × 109/L (17) to 54 × 109/L (60) 24 hours after starting sutimlimab, maintaining ≥50 × 109/L throughout part A. Five patients (42%) achieved durable platelet count responses (≥50 × 109/L in ≥50% of follow-up visits) and 4 achieved complete response (platelet count ≥100 × 109/L). The mean platelet count returned to baseline during washout and increased upon retreatment in part B. The mean platelet count improvements accompanied the rapid inhibition of the classical pathway. There were 74 treatment-emergent adverse events in part A (n = 10) and 70 in part B (n = 6). Five serious adverse events were observed; 1 event (migraine) was assessed by the investigator as related to sutimlimab. These results demonstrated that in some patients with ITP, autoantibodies activate the classical complement pathway, accelerating platelet destruction or impairing platelet production and contributing to treatment failure. Thus, C1s inhibition may be a safe and beneficial therapeutic approach for patients with chronic/refractory ITP.
慢性/难治性免疫性血小板减少症 (ITP) 是一种罕见且病理生理异质性疾病,对现有治疗方法的反应各不相同。Sutimlimab 是一种首创的人源化单克隆抗 C1s IgG4 抗体,可选择性抑制经典途径。这项 1 期研究 (NCT03275454) 评估了每周两次 sutimlimab 在对 ≥2 种治疗反应不足(血小板计数 ≤ 30×109/L)的慢性/难治性 ITP 患者中的安全性、疗效、药代动力学和药效学。12 名患者(中位年龄 42 岁)接受 sutimlimab 治疗,中位时间为 20.5 周,随后中位洗脱期为 2 周(第 A 部分)。在第 B 部分中,12 名符合条件的患者中有 7 名接受了 sutimlimab 重新治疗,中位时间为 113 周。在第 A 部分中,开始 sutimlimab 后 24 小时,血小板计数的平均值(标准差)从 25×109/L(17)增加到 54×109/L(60),整个第 A 部分均维持≥50×109/L。5 名患者(42%)获得持久的血小板计数反应(≥50×109/L 在≥50%的随访中),4 名患者获得完全反应(血小板计数≥100×109/L)。洗脱期内血小板计数恢复至基线,第 B 部分重新治疗时增加。血小板计数的平均改善伴随着经典途径的快速抑制。第 A 部分(n=10)和第 B 部分(n=6)分别有 74 次治疗相关不良事件。观察到 5 起严重不良事件;研究者评估 1 起事件(偏头痛)与 sutimlimab 相关。这些结果表明,在一些 ITP 患者中,自身抗体激活经典补体途径,加速血小板破坏或损害血小板生成,并导致治疗失败。因此,C1s 抑制可能是治疗慢性/难治性 ITP 患者的一种安全且有益的治疗方法。
