皮肤病和非皮肤病病症中司泊利单抗试验的预设安全事件分析。
Analysis of Predefined Safety Events Across Spesolimab Trials in Dermatological and Non-Dermatological Conditions.
作者信息
Gordon Kenneth B, Tada Yayoi, Anadkat Milan J, Choon Siew Eng, Elewski Boni, Barker Jonathan N, Mostaghimi Arash, Eyerich Kilian, Tang Ming, Haeufel Thomas, Thoma Christian, Thaçi Diamant
机构信息
Department of Dermatology, Medical College of Wisconsin, Milwaukee, WI, USA.
Department of Dermatology, Teikyo University School of Medicine, Tokyo, Japan.
出版信息
Dermatol Ther (Heidelb). 2025 Feb;15(2):395-411. doi: 10.1007/s13555-024-01325-7. Epub 2025 Feb 10.
INTRODUCTION
Spesolimab, a selective, humanised monoclonal antibody targeting the interleukin-36 receptor, is approved for the treatment of generalised pustular psoriasis (GPP). As a result of the limited patient numbers in GPP trials of spesolimab, analysing safety events across dermatological and non-dermatological diseases helps to further characterise the known safety profile of spesolimab. Here, we analyse predefined safety events from nine randomised, placebo-controlled spesolimab trials across dermatological (including GPP) and gastrointestinal conditions.
METHODS
Predefined safety events were based on the known safety profile of spesolimab across all diseases investigated to date and potential risks of biological therapeutics, and included serious/severe/opportunistic infections, hypersensitivity, malignancies and peripheral neuropathy.
RESULTS
Including placebo-controlled trials and open-label periods/trials, 589 patients received ≥ 1 dose of spesolimab (772.2 patient-years; mean exposure 1.31 patient-years). Overall, 452 patients had long-term exposure (≥ 6 months) to spesolimab, with 31 patients up to ≥ 3 years. In placebo-controlled periods, 445 patients had exposure to spesolimab (162.0 patient-years; mean exposure 0.36 patient-years). Severe/serious/opportunistic infections occurred in 0-3.2% of spesolimab-treated patients and 0-14.3% of placebo-treated patients. Malignancies occurred infrequently across trials (0-6.7% in spesolimab, 0-2.3% in placebo). Peripheral neuropathy events also occurred infrequently, with single events reported in the placebo arm of EFFISAYIL 2, and the spesolimab and placebo arms of palmoplantar pustulosis Study 2. Potential hypersensitivity events occurred in all trials, except for Crohn's disease, and were largely balanced between spesolimab (7.7-33.3%) and placebo (4.3-44.4%).
CONCLUSIONS
Across placebo-controlled periods of spesolimab trials in dermatological and non-dermatological conditions, severe/serious/opportunistic infections, malignancies and peripheral neuropathy events were low, with no evidence for an increased risk with spesolimab versus placebo. Potential hypersensitivity events were similar between spesolimab and placebo. These results support the favourable safety profile of spesolimab observed in EFFISAYIL 2, the largest GPP trial conducted to date.
引言
司泊利单抗是一种靶向白细胞介素-36受体的选择性人源化单克隆抗体,已被批准用于治疗泛发性脓疱型银屑病(GPP)。由于司泊利单抗治疗GPP的试验中患者数量有限,分析皮肤科和非皮肤科疾病中的安全事件有助于进一步明确司泊利单抗已知的安全性特征。在此,我们分析了司泊利单抗在9项针对皮肤科(包括GPP)和胃肠道疾病的随机、安慰剂对照试验中预先定义的安全事件。
方法
预先定义的安全事件基于司泊利单抗在迄今所有研究疾病中的已知安全性特征以及生物治疗药物的潜在风险,包括严重/重度/机会性感染、超敏反应、恶性肿瘤和周围神经病变。
结果
纳入安慰剂对照试验以及开放标签期/试验,589例患者接受了≥1剂司泊利单抗(772.2患者年;平均暴露时间1.31患者年)。总体而言,452例患者长期暴露(≥6个月)于司泊利单抗,其中31例患者暴露时间长达≥3年。在安慰剂对照期,445例患者暴露于司泊利单抗(162.0患者年;平均暴露时间0.36患者年)。在接受司泊利单抗治疗的患者中,严重/重度/机会性感染发生率为0 - 3.2%,在接受安慰剂治疗的患者中为0 - 14.3%。在各试验中,恶性肿瘤发生率较低(司泊利单抗组为0 - 6.7%,安慰剂组为0 - 2.3%)。周围神经病变事件也较少发生,在EFFISAYIL 2的安慰剂组以及掌跖脓疱病研究2的司泊利单抗组和安慰剂组均有单例事件报告。除克罗恩病外,所有试验中均出现了潜在的超敏反应事件,且在司泊利单抗组(7.7 - 33.3%)和安慰剂组(4.3 - 44.4%)之间基本平衡。
结论
在司泊利单抗治疗皮肤科和非皮肤科疾病的安慰剂对照期内,严重/重度/机会性感染、恶性肿瘤和周围神经病变事件发生率较低,没有证据表明司泊利单抗与安慰剂相比风险增加。司泊利单抗和安慰剂之间潜在的超敏反应事件相似。这些结果支持了在迄今为止开展的最大规模GPP试验EFFISAYIL 2中观察到的司泊利单抗良好的安全性特征。
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