Division of Pediatric Endocrinology, Department of Pediatrics, WakeMed Children's Hospital, Raleigh, North Carolina, USA.
Clinical Development, Grifols Therapeutics Inc. Research Triangle Park, North Carolina, USA.
Pediatr Diabetes. 2021 Mar;22(2):192-201. doi: 10.1111/pedi.13162. Epub 2020 Dec 13.
While circulating levels of alpha -proteinase inhibitor (alpha -PI) are typically normal, antiprotease activity appears to be compromised in patients with Type 1 diabetes mellitus (T1DM). Because alpha -PI [human] (alpha -PI[h]) therapy can inhibit pro-inflammatory mediators associated with β-cell destruction and reduced insulin production, it has been proposed for T1DM disease prevention. The aim of this study was to evaluate safety, tolerability, and efficacy of intravenous (IV) alpha -PI[h] in preserving C-peptide production in newly diagnosed T1DM patients.
Seventy-six participants (aged 6-35 years) were randomized at 25 centers within 3 months of T1DM diagnosis.
A Phase II, multicenter, partially blinded, placebo-controlled, proof-of-concept study evaluating four dosing regimens of alpha -PI[h] (NCT02093221, GTI1302): weekly IV infusions of either 90 or 180 mg/kg, each for either 13 or 26 weeks. Safety and efficacy were monitored over 52 weeks with an efficacy evaluation planned at 104 weeks. The primary efficacy endpoint was change from baseline in the 2-h area-under-the-curve C-peptide level from a mixed-meal tolerance test at 52 weeks. A battery of laboratory tests, including inflammatory biomarkers, constituted exploratory efficacy variables.
Infusions were well tolerated with no new safety signals. All groups exhibited highly variable declines in the primary outcome measure at 52 weeks with no statistically significant difference from placebo. Interleukin-6 (IL-6) was reduced from baseline in all alpha -PI treatment groups but not the placebo group.
Pharmacologic therapy with alpha -PI[h] is safe, well tolerated, and able to reduce IL-6 levels; however, due to variability in the efficacy endpoint, its effects on preservation of C-peptide production were inconclusive.
尽管α-蛋白酶抑制剂(α-PI)的循环水平通常正常,但 1 型糖尿病(T1DM)患者的抗蛋白酶活性似乎受损。由于α-PI[人](α-PI[h])治疗可以抑制与β细胞破坏和胰岛素产生减少相关的促炎介质,因此它被提议用于 T1DM 疾病预防。本研究的目的是评估静脉内(IV)α-PI[h]在保护新诊断的 T1DM 患者 C 肽产生方面的安全性、耐受性和疗效。
76 名参与者(年龄 6-35 岁)在 T1DM 诊断后 3 个月内在 25 个中心随机分组。
一项评估 α-PI[h]四种给药方案(NCT02093221,GTI1302)的 II 期、多中心、部分盲法、安慰剂对照、概念验证研究:每周静脉输注 90 或 180mg/kg,分别为 13 或 26 周。在 52 周内监测安全性和疗效,并计划在 104 周时进行疗效评估。主要疗效终点是 52 周时混合餐耐量试验中 2 小时 C 肽曲线下面积的基线变化。一系列实验室检查,包括炎症生物标志物,构成了探索性疗效变量。
输注耐受良好,无新的安全信号。所有组在 52 周时主要结局指标均表现出高度可变的下降,与安慰剂相比无统计学差异。所有α-PI 治疗组的白细胞介素-6(IL-6)均从基线下降,但安慰剂组没有。
α-PI[h]的药物治疗安全、耐受性好,能够降低 IL-6 水平;然而,由于疗效终点的变异性,其对 C 肽产生的保护作用尚无定论。
