E-52862——一种选择性σ-1受体拮抗剂,用于治疗外周神经性疼痛:两项针对慢性术后疼痛和疼痛性糖尿病神经病变患者的随机、双盲2期研究。
E-52862-A selective sigma-1 receptor antagonist, in peripheral neuropathic pain: Two randomized, double-blind, phase 2 studies in patients with chronic postsurgical pain and painful diabetic neuropathy.
作者信息
Gálvez Rafael, Mayoral Victor, Cebrecos Jesús, Medel Francisco J, Morte Adelaida, Sust Mariano, Vaqué Anna, Montes-Pérez Antonio, Neira-Reina Fernando, Cánovas Luz, Margarit César, Bouhassira Didier
机构信息
Pain Clinic, Virgen de Las Nieves University Hospital, Granada, Spain.
Bellvitge University Hospital, L'Hospitalet de Llobregat, Barcelona, Spain.
出版信息
Eur J Pain. 2025 Jan;29(1). doi: 10.1002/ejp.4755.
BACKGROUND
We report the efficacy and safety of E-52862-a selective, sigma-1 receptor antagonist-from phase 2, randomized, proof-of-concept studies in patients with moderate-to-severe, neuropathic, chronic postsurgical pain (CPSP) and painful diabetic neuropathy (PDN).
METHODS
Adult patients (CPSP [N = 116]; PDN [N = 163]) were randomized at a 1:1 ratio to 4 weeks of treatment with E-52862 (CPSP [n = 55]; PDN [n = 85]) or placebo (CPSP [n = 61]; PDN [n = 78]) orally once daily. Pain intensity scores were measured using a numerical pain rating scale from 0 (no pain) to 10 (worst pain imaginable). The primary analysis population comprised patients who received study drug with ≥1 baseline and on-treatment observation (full analysis set).
RESULTS
In CPSP, mean baseline average pain was 6.2 for E-52862 vs. 6.5 for placebo. Week 4 mean change from baseline (CFB) for average pain was -1.6 for E-52862 vs. -0.9 for placebo (least squares mean difference [LSMD]: -0.9; p = 0.029). In PDN, mean baseline average pain was 5.3 for E-52862 vs. 5.4 for placebo. Week 4 mean CFB for average pain was -2.2 for E-52862 vs. -2.1 for placebo (LSMD: -0.1; p = 0.766). Treatment-emergent adverse events (TEAEs) were reported in 90.9% of E-52862-treated patients vs. 76.7% of placebo-treated patients in CPSP and 34.1% vs. 26.9% in PDN. Serious TEAEs occurred in CPSP only: E-52862: 5.5%; placebo: 6.7%.
CONCLUSIONS
E-52862 demonstrated superior relief of CPSP vs. placebo after 4 weeks. Reductions in pain intensity were seen in PDN with E-52862; high placebo response rates may have prevented differentiation between treatments. E-52862 had acceptable tolerability in both populations.
SIGNIFICANCE STATEMENT
These proof-of-concept studies validate the mode of action of E-52862, a selective sigma-1 receptor antagonist. In CPSP, E-52862 resulted in clinically meaningful pain relief. In PDN, reductions in pain intensity were seen with E-52862; high placebo response rates may have prevented differentiation between E-52862 and placebo. These findings are clinically relevant given that neuropathic pain is highly incapacitating, lacking effective treatments and representing a significant unmet medical need, and support further development of sigma-1 receptor antagonists for peripheral neuropathic pain.
背景
我们报告了E-52862(一种选择性σ-1受体拮抗剂)在中度至重度神经性慢性术后疼痛(CPSP)和疼痛性糖尿病神经病变(PDN)患者中进行的2期随机概念验证研究的疗效和安全性。
方法
成年患者(CPSP [N = 116];PDN [N = 163])按1:1的比例随机分组,接受E-52862治疗4周(CPSP [n = 55];PDN [n = 85])或安慰剂治疗(CPSP [n = 61];PDN [n = 78]),每日口服一次。使用从0(无疼痛)到10(可想象的最严重疼痛)的数字疼痛评分量表测量疼痛强度评分。主要分析人群包括接受研究药物且有≥1次基线和治疗期观察的患者(全分析集)。
结果
在CPSP中,E-52862组的平均基线平均疼痛为6.2,安慰剂组为6.5。第4周时,E-52862组平均疼痛较基线的变化(CFB)为-1.6,安慰剂组为-0.9(最小二乘均值差异[LSMD]:-0.9;p = 0.029)。在PDN中,E-52862组的平均基线平均疼痛为5.3,安慰剂组为5.4。第4周时,E-52862组平均疼痛CFB为-2.2,安慰剂组为-2.1(LSMD:-0.1;p = 0.766)。CPSP中,90.9%接受E-52862治疗的患者报告了治疗中出现的不良事件(TEAE),安慰剂治疗患者为76.7%;PDN中分别为34.1%和26.9%。严重TEAE仅在CPSP中出现:E-52862组:5.5%;安慰剂组:6.7%。
结论
4周后,E-52862在缓解CPSP方面表现出优于安慰剂的效果。E-52862可降低PDN患者的疼痛强度;高安慰剂反应率可能阻碍了不同治疗方法间的区分。E-52862在两组人群中均具有可接受的耐受性。
意义声明
这些概念验证研究验证了选择性σ-1受体拮抗剂E-52862的作用模式。在CPSP中,E-52862带来了具有临床意义的疼痛缓解。在PDN中,E-52862可降低疼痛强度;高安慰剂反应率可能阻碍了E-52862与安慰剂之间的区分。鉴于神经性疼痛极具致残性、缺乏有效治疗方法且存在重大未满足的医疗需求,这些发现具有临床相关性,并支持进一步开发用于治疗周围神经性疼痛的σ-1受体拮抗剂。
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