S43 Results from the STAR-COVID19 trial, a double-blind RCT of stabilised, synthetic sulforaphane in hospitalised patients with suspected COVID19

‘The fast and the furious’ – Clinical studies in COVID-19 Pub Date : 2022-11-01 DOI:10.1136/thorax-2022-btsabstracts.49

M. Long, H. Abo-Leyah, Y. Giam, T. Vadiveloo, R. Hull, H. Keir, T. Pembridge, D. Alferes De Lima, B. New, S. Inglis, A. Gilmour, C. Hughes, L. Delgado, G. Maclennan, AT Dinkova-Kostova, J. Chalmers

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Abstract

Introduction and ObjectivesThe transcription factor, Nrf2, can directly promote beneficial anti-oxidant and anti-inflammatory responses. In the STAR-COVID19 trial, hospitalised patients with confirmed or suspected COVID19 were treated with stabilised, synthetic sulforaphane (S-SFN)—an Nrf2 inducer—to evaluate impact on clinical status and systemic inflammation.MethodsDouble-blind, randomised, placebo-controlled trial of S-SFN (300 mg S-SFN or placebo once daily for 14 days;allocation ratio 1:1;EudraCT 2020–003486-19) in Dundee, UK. Inclusion criteria were age ≥18 years, suspected or confirmed COVID19 or pneumonia and CURB65 score ≥1. The primary outcome was the 7-point WHO Clinical Status scale at day 15. Secondary outcomes included time to clinical improvement, length of hospital stay, and mortality. Blood samples were taken on days 1, 8 and 15 for exploratory analyses. To assess Nrf2 activity and inflammation, 45 serum cytokines were measured using the Olink Target48 panel and mRNA sequencing of peripheral blood leukocytes performed. Further, as key immune cells in COVID19 responses, select neutrophil functions such as migration, phagocytosis and extracellular trap formation were evaluated.Results133 participants (77.4% PCR-confirmed SARS-CoV-2 infection) were randomized from Nov 2020 to May 2021. 68 received placebo (61.8% male;age 63.6±13.8) and 65 received S-SFN (53.8% male;age 61.6±12.7).S-SFN treatment did not improve clinical status at day 15 (Intention-to-treat population;adjusted OR 0.87, 95%CI 0.41–1.83, p=0.712) and the trial was terminated due to futility. Time to clinical improvement (adjusted HR 1.02(0.70–1.49)), length of hospital stay (aHR 0.84(0.56–1.26)), or 29-day mortality (aHR 1.45(0.67–3.16)) were not improved with S-SFN treatment.230 samples in total were utilised for serum cytokine measurement;Nrf2 targets implicated in cytokine storm, including IL6, IL1β and TNFα, were not significantly changed by S-„SFN treatment. Interestingly, serum TGFα was significantly increased at day 15 in those receiving S-SFN compared with placebo (p=0.004;linear mixed effects model). S-SFN treatment did not significantly affect neutrophil functions investigated.ConclusionS-SFN treatment did not improve clinical status at day 15 or modulate key inflammatory cytokines—however, changes in other factors were indicated. Further analyses, including transcriptomics, to delineate drug activity are currently ongoing.

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star - covid - 19试验的结果，这是一项双盲随机对照试验，在疑似covid - 19住院患者中使用稳定的合成萝卜硫素

转录因子Nrf2可以直接促进有益的抗氧化和抗炎反应。在star - covid - 19试验中，确诊或疑似covid - 19的住院患者接受稳定的合成萝卜硫素(S-SFN)治疗，以评估其对临床状态和全身炎症的影响。方法:在英国邓迪进行双盲、随机、安慰剂对照试验，S-SFN (300 mg S-SFN或安慰剂，每天1次，持续14天;分配比例1:1;EudraCT 2020-003486-19)。纳入标准为年龄≥18岁，疑似或确诊covid - 19或肺炎，且CURB65评分≥1。主要终点是第15天的7分WHO临床状态量表。次要结局包括到临床改善的时间、住院时间和死亡率。在第1、8和15天采集血样进行探索性分析。为了评估Nrf2活性和炎症，使用Olink Target48面板测量45种血清细胞因子，并对外周血白细胞进行mRNA测序。此外，作为covid - 19应答的关键免疫细胞，中性粒细胞的迁移、吞噬和细胞外陷阱形成等功能被评估。结果从2020年11月至2021年5月，133名参与者(77.4%为pcr确诊的SARS-CoV-2感染)被随机分配。安慰剂组68例(男性61.8%，年龄63.6±13.8岁)，S-SFN组65例(男性53.8%，年龄61.6±12.7岁)。S-SFN治疗在第15天没有改善临床状况(意向治疗人群;调整OR 0.87, 95%CI 0.41-1.83, p=0.712)，试验因无效而终止。S-SFN治疗未改善临床改善时间(调整HR 1.02(0.70-1.49))、住院时间(aHR 0.84(0.56-1.26))或29天死亡率(aHR 1.45(0.67-3.16))。总共有230个样本用于血清细胞因子测量，与细胞因子风暴有关的Nrf2靶点，包括IL6、IL1β和TNFα，在S-“SFN”处理下没有显著改变。有趣的是，与安慰剂相比，接受S-SFN的患者在第15天血清tgf - α显著升高(p=0.004;线性混合效应模型)。S-SFN治疗对所研究的中性粒细胞功能没有显著影响。结论s - sfn治疗并没有改善第15天的临床状况，也没有调节关键的炎症细胞因子，但表明其他因素发生了变化。目前正在进行进一步的分析，包括转录组学，以描述药物活性。

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‘The fast and the furious’ – Clinical studies in COVID-19

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