微生物组疗法SER-109治疗复发性CDI的3期综合安全性分析

Matthew Sims, Charles Berenson, Stuart Cohen, Elaine Wang, Elizabeth Hohmann, Richard Nathan, Alberto Odio, Paul Cook, Kelly Brady, David Lombardi, Asli Memisoglu, Ananya De, Brooke Hasson, Bret Lashner, Louis Korman, Doria Grimard, Juan Carlos Moises Gutierrez, Barbara McGovern, Lisa Von Moltke
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Methods: ECOSPOR III was a double-blind, placebo-controlled trial conducted in participants with ≥2 CDI recurrences randomized 1:1 to placebo or SER-109. ECOSPOR IV was an open-label, single-arm study conducted in 263 patients with rCDI enrolled in 2 cohorts: (1) rollover participants from ECOSPOR III with on-study recurrence and (2) participants with ≥1 CDI recurrence, inclusive of the current episode. In both studies, the investigational product was administered as 4 oral capsules over 3 days. Treatment-emergent adverse events (TEAEs) were collected through week 8; serious TEAEs and TEAEs of special interest (ie, bacteremia, abscess, meningitis) were collected through week 24. Results: In total, 349 participants received SER-109 in ECOSPOR III and/or ECOSPOR IV (mean age 64.2; 68.8% female). Chronic diseases included cardiac disease (31.2%), immunocompromised or immunosuppressed (21.2%), diabetes (18.9% ), and renal impairment or failure (13.2%). Overall, 221 (63.3%) of 349 participants who received SER-109 experienced TEAEs through week 24. Most were mild to moderate and gastrointestinal. The most common (>5% of participants) treatment related TEAEs were flatulence, abdominal pain and distension, decreased appetite, constipation, nausea, fatigue, and diarrhea. No participants experienced a treatment-related TEAE leading to study withdrawal. Invasive infections were observed in 28 participants (8%); those with identified pathogens were unrelated to SER-109 species, and all were deemed unrelated to treatment by the investigators. There were 11 deaths (3.2%) and 48 participants (13.8%) with serious TEAEs, none of which were deemed treatment related. There were no clinically important differences in the safety profile across subgroups of sex, race, prior antibiotic regimen, or number of CDI recurrences. No safety signals were observed in participants with renal impairment or failure, diabetes, cardiac disease, or immunocompromised or immunosuppressed individuals. Conclusions: In this integrated analysis of phase 3 trials, SER-109, an investigational microbiome therapeutic, was well tolerated in this vulnerable patient population with prevalent comorbidities. No infections, nor those with identified pathogens, were attributed to SER-109 or product species. This safety profile might be expected because this purified product is composed of spore-forming Firmicutes normally abundant in the healthy microbiome. Financial support: This study was funded by Seres Therapeutics. 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引用次数: 0

摘要

背景:艰难梭菌感染(CDI)常复发于年龄≥65岁及有合并症的患者。临床试验通常排除有免疫抑制史、恶性肿瘤、肾功能不全或其他合并症的患者。在一项3期试验(ECOSPOR III)中,SER-109在降低第8周复发性CDI (rCDI)风险方面优于安慰剂,并且耐受性良好。我们报告了从3期研究ECOSPOR III和ECOSPOR IV到24周的广泛患者群体中SER-109的综合安全性数据。方法:ECOSPOR III是一项双盲,安慰剂对照试验,在≥2例CDI复发的参与者中进行,随机1:1分配到安慰剂或SER-109。ECOSPOR IV是一项开放标签单臂研究,纳入263例rCDI患者,分为2个队列:(1)ECOSPOR III研究中复发的患者,(2)CDI复发≥1次的患者,包括当前发作。在这两项研究中,研究产品以4粒口服胶囊的形式在3天内服用。收集治疗不良事件(teae)至第8周;收集严重teae和特殊teae(如菌血症、脓肿、脑膜炎)至第24周。结果:总共有349名参与者在ECOSPOR III和/或ECOSPOR IV中接受SER-109治疗(平均年龄64.2;68.8%的女性)。慢性疾病包括心脏病(31.2%)、免疫功能低下或免疫抑制(21.2%)、糖尿病(18.9%)和肾损害或肾功能衰竭(13.2%)。总体而言,349名接受SER-109治疗的参与者中,221名(63.3%)在第24周经历了teae。大多数是轻度到中度的胃肠道疾病。最常见的(5%的参与者)与治疗相关的teae是肠胃胀气、腹痛和腹胀、食欲下降、便秘、恶心、疲劳和腹泻。没有参与者经历与治疗相关的TEAE导致研究退出。侵袭性感染28例(8%);那些鉴定出病原体的人与SER-109物种无关,并且所有人都被调查人员认为与治疗无关。11例死亡(3.2%)和48例严重teae(13.8%),均与治疗无关。在性别、种族、既往抗生素治疗方案或CDI复发次数等亚组中,安全性无临床重要差异。在肾损害或肾功能衰竭、糖尿病、心脏病、免疫功能低下或免疫抑制的受试者中未观察到安全信号。结论:在这项3期试验的综合分析中,SER-109,一种研究性微生物组治疗药物,在这一易受感染的普遍合并症患者群体中具有良好的耐受性。没有感染,也没有确定的病原体,归因于SER-109或产品种类。这种安全性是意料之中的,因为这种纯化产品是由健康微生物群中通常丰富的形成孢子的厚壁菌门组成的。资金支持:本研究由Seres Therapeutics资助。披露:没有
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Integrated safety analysis of phase 3 studies for investigational microbiome therapeutic, SER-109, in recurrent CDI
Background: Clostridioides difficile infection (CDI) often recurs in patients aged ≥65 years and those with comorbidities. Clinical trials often exclude patients with history of immunosuppression, malignancy, renal insufficiency, or other comorbidities. In a phase 3 trial (ECOSPOR III), SER-109 was superior to placebo in reducing recurrent CDI (rCDI) risk at week 8 and was well tolerated. We report integrated safety data for SER-109 in a broad patient population through week 24 from phase 3 studies: ECOSPOR III and ECOSPOR IV. Methods: ECOSPOR III was a double-blind, placebo-controlled trial conducted in participants with ≥2 CDI recurrences randomized 1:1 to placebo or SER-109. ECOSPOR IV was an open-label, single-arm study conducted in 263 patients with rCDI enrolled in 2 cohorts: (1) rollover participants from ECOSPOR III with on-study recurrence and (2) participants with ≥1 CDI recurrence, inclusive of the current episode. In both studies, the investigational product was administered as 4 oral capsules over 3 days. Treatment-emergent adverse events (TEAEs) were collected through week 8; serious TEAEs and TEAEs of special interest (ie, bacteremia, abscess, meningitis) were collected through week 24. Results: In total, 349 participants received SER-109 in ECOSPOR III and/or ECOSPOR IV (mean age 64.2; 68.8% female). Chronic diseases included cardiac disease (31.2%), immunocompromised or immunosuppressed (21.2%), diabetes (18.9% ), and renal impairment or failure (13.2%). Overall, 221 (63.3%) of 349 participants who received SER-109 experienced TEAEs through week 24. Most were mild to moderate and gastrointestinal. The most common (>5% of participants) treatment related TEAEs were flatulence, abdominal pain and distension, decreased appetite, constipation, nausea, fatigue, and diarrhea. No participants experienced a treatment-related TEAE leading to study withdrawal. Invasive infections were observed in 28 participants (8%); those with identified pathogens were unrelated to SER-109 species, and all were deemed unrelated to treatment by the investigators. There were 11 deaths (3.2%) and 48 participants (13.8%) with serious TEAEs, none of which were deemed treatment related. There were no clinically important differences in the safety profile across subgroups of sex, race, prior antibiotic regimen, or number of CDI recurrences. No safety signals were observed in participants with renal impairment or failure, diabetes, cardiac disease, or immunocompromised or immunosuppressed individuals. Conclusions: In this integrated analysis of phase 3 trials, SER-109, an investigational microbiome therapeutic, was well tolerated in this vulnerable patient population with prevalent comorbidities. No infections, nor those with identified pathogens, were attributed to SER-109 or product species. This safety profile might be expected because this purified product is composed of spore-forming Firmicutes normally abundant in the healthy microbiome. Financial support: This study was funded by Seres Therapeutics. Disclosures: None
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