Allergy Associates of the Palm Beaches, North Palm Beach, FL, United States.
Department of Medicine, Laval University, Québec City, QC, Canada.
Front Immunol. 2021 Jul 8;12:707463. doi: 10.3389/fimmu.2021.707463. eCollection 2021.
We report here the results of a phase 3 study to assess the efficacy, safety, and tolerability of GC5107, a new 10% liquid intravenous immunoglobulin (IVIG) in preventing serious bacterial infections in patients with primary immunodeficiency (ClinicalTrials.gov: NCT02783482). Over a 12-month study period, 49 patients aged 3 to 70 years with a confirmed diagnosis of primary immunodeficiency received GC5107 at doses ranging from 319 to 881 mg/kg body weight every 21 or 28 days, according to their previous IVIG maintenance therapy. A total of 667 infusions of GC5107 were administered comprising a total of 45.86 patient-years of treatment. A single acute serious bacterial infection occurred during the study, resulting in an incidence of 0.02 events per patient-year (upper 99% one-sided confidence interval limit: 0.21), meeting the prespecified primary efficacy endpoint. The mean incidence of infections other than acute serious bacterial infections was 2.9 infections per patient-year. Efficacy was also demonstrated by the low mean annualized rate of hospitalizations due to infection (0.1 day) and the mean annualized duration of hospitalizations (0.1 day). The mean rate of intravenous and oral antibiotic use was 0.1 day and 13.2 days, respectively. There was a mean of 7.1 days of missed work, school, or daycare days. The proportion of infusions with temporally associated adverse events (TAAEs) occurring during or within 72 hours after GC5107 infusion was 0.24 (upper 95% one-sided confidence interval limit: 0.31), meeting the pre-specified primary safety endpoint. Overall, 149 of 667 infusions (22%) were associated with TAAEs. The most common TAAE was headache, reported by 49% of patients. More than 98% (731/743) of all adverse events that occurred throughout the 12-month study period were mild or moderate. More than 98% of infusions were completed without discontinuation, interruption or rate reduction. There were no treatment-emergent serious adverse events related to GC5107 or study discontinuations due to an adverse event. Overall, pharmacokinetic parameters for GC5107 were within the range of those reported in studies of other marketed IVIG products. Results of the present study demonstrate that GC5107 is an effective, safe and well-tolerated treatment for patients with primary immunodeficiency.
我们在此报告一项 3 期研究的结果,该研究旨在评估新型 10%液体静脉注射免疫球蛋白(IVIG)GC5107 预防原发性免疫缺陷患者严重细菌感染的疗效、安全性和耐受性(ClinicalTrials.gov:NCT02783482)。在为期 12 个月的研究期间,49 名年龄在 3 至 70 岁的确诊原发性免疫缺陷患者根据其之前的 IVIG 维持治疗,接受了 319 至 881mg/kg 体重的 GC5107 剂量,每 21 或 28 天一次。共给予了 667 次 GC5107 输注,共治疗了 45.86 患者年。在研究期间发生了 1 次急性严重细菌感染,导致感染发生率为 0.02 例/患者年(99%单侧置信区间上限:0.21),符合预设的主要疗效终点。除急性严重细菌感染以外的感染的平均发生率为 2.9 例/患者年。由于感染导致的平均每年住院率(0.1 天)和平均每年住院时间(0.1 天)也较低,这也证明了疗效。平均每年因感染而使用静脉和口服抗生素的天数分别为 0.1 天和 13.2 天。平均有 7.1 天的工作、上学或日托缺勤。输注期间或输注后 72 小时内出现与输注相关的不良事件(TAAEs)的输注比例为 0.24(95%单侧置信区间上限:0.31),符合预先指定的主要安全性终点。总体而言,667 次输注中有 149 次(22%)与 TAAEs 相关。最常见的 TAAE 是头痛,有 49%的患者报告。整个 12 个月研究期间发生的所有不良事件中,超过 98%(731/743)为轻度或中度。超过 98%的输注无需停药、中断或降低输注速率。没有与 GC5107 相关的治疗突发严重不良事件或因不良事件而停止研究。总体而言,GC5107 的药代动力学参数在其他已上市 IVIG 产品研究报告的范围内。本研究结果表明,GC5107 是一种有效、安全且耐受良好的原发性免疫缺陷患者治疗药物。
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