Grass Center for Bioengineering, Benin School of Computer Science and Engineering, Jerusalem, Israel.
Department of Cell and Developmental Biology, Silberman Institute of Life Sciences, Jerusalem, Israel.
Elife. 2023 Jan 27;12:e79946. doi: 10.7554/eLife.79946.
Viral infection is associated with a significant rewire of the host metabolic pathways, presenting attractive metabolic targets for intervention.
We chart the metabolic response of lung epithelial cells to SARS-CoV-2 infection in primary cultures and COVID-19 patient samples and perform in vitro metabolism-focused drug screen on primary lung epithelial cells infected with different strains of the virus. We perform observational analysis of Israeli patients hospitalized due to COVID-19 and comparative epidemiological analysis from cohorts in Italy and the Veteran's Health Administration in the United States. In addition, we perform a prospective non-randomized interventional open-label study in which 15 patients hospitalized with severe COVID-19 were given 145 mg/day of nanocrystallized fenofibrate added to the standard of care.
SARS-CoV-2 infection produced transcriptional changes associated with increased glycolysis and lipid accumulation. Metabolism-focused drug screen showed that fenofibrate reversed lipid accumulation and blocked SARS-CoV-2 replication through a PPARα-dependent mechanism in both alpha and delta variants. Analysis of 3233 Israeli patients hospitalized due to COVID-19 supported in vitro findings. Patients taking fibrates showed significantly lower markers of immunoinflammation and faster recovery. Additional corroboration was received by comparative epidemiological analysis from cohorts in Europe and the United States. A subsequent prospective non-randomized interventional open-label study was carried out on 15 patients hospitalized with severe COVID-19. The patients were treated with 145 mg/day of nanocrystallized fenofibrate in addition to standard-of-care. Patients receiving fenofibrate demonstrated a rapid reduction in inflammation and a significantly faster recovery compared to patients admitted during the same period.
Taken together, our data suggest that pharmacological modulation of PPARα should be strongly considered as a potential therapeutic approach for SARS-CoV-2 infection and emphasizes the need to complete the study of fenofibrate in large randomized controlled clinical trials.
Funding was provided by European Research Council Consolidator Grants OCLD (project no. 681870) and generous gifts from the Nikoh Foundation and the Sam and Rina Frankel Foundation (YN). The interventional study was supported by Abbott (project FENOC0003).
NCT04661930.
病毒感染会显著改变宿主的代谢途径,为干预提供了有吸引力的代谢靶点。
我们绘制了肺上皮细胞在原发性培养物和 COVID-19 患者样本中对 SARS-CoV-2 感染的代谢反应,并对感染不同病毒株的原代肺上皮细胞进行了体外代谢为重点的药物筛选。我们对因 COVID-19 住院的以色列患者进行了观察性分析,并对意大利和美国退伍军人健康管理局的队列进行了比较流行病学分析。此外,我们进行了一项前瞻性、非随机、干预性、开放性标签研究,其中 15 名因 COVID-19 住院的患者每天给予 145 毫克纳米结晶非诺贝特,加入标准治疗。
SARS-CoV-2 感染导致与糖酵解和脂质积累增加相关的转录变化。以代谢为重点的药物筛选表明,非诺贝特通过 PPARα 依赖机制逆转了脂质积累,并阻断了 alpha 和 delta 变体中的 SARS-CoV-2 复制。对因 COVID-19 住院的 3233 名以色列患者的分析支持了体外研究结果。服用贝特类药物的患者免疫炎症标志物显著降低,恢复更快。来自欧洲和美国队列的比较流行病学分析也得到了进一步证实。随后对 15 名因 COVID-19 住院的严重患者进行了一项前瞻性、非随机、干预性、开放性标签研究。患者在标准治疗的基础上加用每天 145 毫克纳米结晶非诺贝特。与同期入院的患者相比,接受非诺贝特治疗的患者炎症迅速减轻,恢复速度明显加快。
综上所述,我们的数据表明,PPARα 的药理学调节应被强烈考虑作为 SARS-CoV-2 感染的潜在治疗方法,并且强调需要在大型随机对照临床试验中完成非诺贝特的研究。
该研究由欧洲研究理事会巩固者资助 OCLD(项目编号 681870)以及 Nikoh 基金会和 Sam 和 Rina Frankel 基金会(YN)的慷慨捐赠提供。干预性研究得到了 Abbott(项目 FENOC0003)的支持。
NCT04661930。
Zotero 插件
