单菌株疗法 EDP1815 对先天性和适应性免疫挑战反应的免疫调节作用--随机安慰剂对照临床试验。

IF 4.3 3区 材料科学 Q1 ENGINEERING, ELECTRICAL & ELECTRONIC ACS Applied Electronic Materials Pub Date : 2024-08-01 Epub Date: 2024-05-15 DOI:10.1007/s12026-024-09484-7
Boukje C Eveleens Maarse, Micha N Ronner, Manon A A Jansen, Tessa Niemeyer-van der Kolk, Aliede E In 't Veld, Erica S Klaassen, Saira Ahmad, Andrea Itano, Duncan McHale, Matthijs Moerland
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引用次数: 0

摘要

肠道微生物群可调节全身炎症,因此是免疫调节的目标。研究人员以健康参与者为研究对象,研究了EDP1815的免疫调节作用,EDP1815是一种组织胞浆菌(Prevotella histicola)的细菌共生菌株。采用匙孔帽贝血蓝蛋白(KLH)的新抗原挑战评估了对适应性免疫的影响,而采用局部收费样受体 7(TLR7)激动剂咪喹莫特评估了对先天性免疫的影响。对两种肠溶包衣水平(EC1、EC2)的胶囊进行了比较。36名健康参试者接受了每天剂量为8×1010个细胞的EDP1815-EC1、EDP1815-EC2或安慰剂(随机分配1:1:1),为期60天。他们在第 8、24 和 36 天接种 KLH 疫苗,并在第 57 天接受皮内挑战。KLH挑战的结果是抗体水平、皮肤挑战后的皮肤血流量和红斑,通过成像技术进行测量。结果包括与 KLH 挑战类似的成像测量,以及水疱液中炎症细胞和细胞因子的涌入。EDP1815 治疗对 KLH 挑战没有影响,对咪喹莫特挑战的成像结果也没有影响。EDP1815治疗参与者的水疱液中炎症细胞涌入量持续降低(中性粒细胞,p = 0.016;粒细胞,p = 0.024),在EC1中更为明显。EDP1815治疗参与者的水疱液中白细胞介素[IL]-1β、IL-6、IL-8、IL-10、干扰素[IFN]-γ和肿瘤坏死因子的流入量较低。EDP1815对咪喹莫特驱动的先天性免疫反应有免疫调节作用,但对KLH挑战没有影响。试验注册号NCT05682222;日期:2022年7月22日。
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Immunomodulating effects of the single bacterial strain therapy EDP1815 on innate and adaptive immune challenge responses - a randomized, placebo-controlled clinical trial.

The gut microbiome can modulate systemic inflammation and is therefore target for immunomodulation. Immunomodulating effects of EDP1815, a bacterial commensal strain of Prevotella histicola, were studied in healthy participants. Effects on adaptive immunity were evaluated by a neo-antigen challenge with keyhole limpet haemocyanin (KLH), while effects on innate immunity were evaluated by topical toll-like receptor 7 (TLR7) agonist imiquimod. Capsules with two enteric coating levels (EC1, EC2) were compared. Thirty-six healthy participants were included and received a daily dose of 8 × 1010 cells EDP1815-EC1, EDP1815-EC2 or placebo (randomization 1:1:1) for 60 days. They received KLH vaccinations at days 8, 24 and 36, with intradermal skin challenge at day 57. KLH challenge outcomes were antibody levels, and skin blood flow and erythema after skin challenge, measured by imaging techniques. Imiquimod administration started at day 57, for 72 h. Outcomes consisted of imaging measurements similar to the KLH challenge, and the influx of inflammatory cells and cytokines in blister fluid. There was no effect of EDP1815 treatment on the KLH challenge, neither on the imaging outcomes of the imiquimod challenge. There was a consistently lower influx of inflammatory cells in the blister fluid of EDP1815-treated participants (neutrophils, p = 0.016; granulocytes, p = 0.024), more pronounced in EC1. There was a lower influx of interleukin [IL]-1β, IL-6, IL-8, IL-10, interferon [IFN]-γ and tumour necrosis factor in blister fluid of EDP1815-treated participants. EDP1815 had immunomodulatory effects on the innate immune response driven by imiquimod, but no effect on the KLH challenge was observed. Trial registration number: NCT05682222; date: 22 July 2022.

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