通过调节循环炎症细胞因子探索脓毒症的脂质修饰疗法:一项孟德尔随机化研究
Exploring lipid-modifying therapies for sepsis through the modulation of circulating inflammatory cytokines: a Mendelian randomization study.
作者信息
Li Quan, Qu Yun, Xue Jinfang, Kang Hai, Lyu Chuanzhu
机构信息
1Department of Emergency Medicie, Yantai Yuhuangding Hospital of Qingdao University, Yantai 264000, China.
2Emergency Department, the State Key Laboratory for Complex, Severe and Rare Diseases, Peking Union Medical College Hospital, Chinese Academy of Medical Science and Peking Union Medical College, Beijing 100730, China.
出版信息
World J Emerg Med. 2025 May 1;16(3):256-261. doi: 10.5847/wjem.j.1920-8642.2025.045.
BACKGROUND
Whether lipid-modifying drugs directly impact the outcome of sepsis remains uncertain. Therefore, systematic investigations are needed to explore the potential impact of lipid-related therapies on sepsis outcomes and to elucidate the underlying mechanisms involving circulating inflammatory cytokines, which may play critical roles in the pathogenesis of sepsis. This study aimed to utilize drug-target Mendelian randomization to assess the direct causal effects of genetically proxied lipid-modifying therapies on sepsis outcomes.
METHODS
First, a two-sample Mendelian randomization study was conducted to validate the causal associations among high-density lipoprotein cholesterol (HDL-C), low-density lipoprotein cholesterol (LDL-C), and sepsis. A subsequent drug-target Mendelian randomization study assessed the direct causal effects of genetically proxied lipid-modifying therapies on the risk of sepsis, sepsis-related critical care admission, and sepsis-related death. The identified lipid-modifying drug targets were subsequently explored for direct causal relationships with 36 circulating inflammatory cytokines. Finally, enrichment analyses of the identified cytokines were conducted to explore the potential relationships of lipid-modifying drugs with the inflammatory response.
RESULTS
Genetically proxied cholesteryl ester transfer protein (CETP) inhibitors were significantly associated with sepsis-related critical care admission (=0.84, 95% [0.74, 0.95], =0.008,) and sepsis-related death (=0.68, 95% [0.52, 0.88], =0.004). The genetically proxied CETP inhibitors were strongly associated with the levels of 15 circulating inflammatory cytokines. Enrichment analyses indicated that CETP inhibitors may modulate inflammatory cytokines and influence the inflammatory response pathway.
CONCLUSION
This study supports a causal effect of genetically proxied CETP inhibitors in reducing the risk of sepsis-related critical care admission and death. These findings suggest that the underlying mechanism may involve the modulation of some circulating inflammatory cytokines, influencing the inflammatory response pathway.
背景
降脂药物是否直接影响脓毒症的结局仍不确定。因此,需要进行系统研究以探讨脂质相关疗法对脓毒症结局的潜在影响,并阐明涉及循环炎症细胞因子的潜在机制,这些细胞因子可能在脓毒症的发病机制中起关键作用。本研究旨在利用药物靶点孟德尔随机化来评估基因代理的降脂疗法对脓毒症结局的直接因果效应。
方法
首先,进行了一项两样本孟德尔随机化研究,以验证高密度脂蛋白胆固醇(HDL-C)、低密度脂蛋白胆固醇(LDL-C)与脓毒症之间的因果关联。随后的药物靶点孟德尔随机化研究评估了基因代理的降脂疗法对脓毒症风险、脓毒症相关重症监护入院和脓毒症相关死亡风险的直接因果效应。随后探索已确定的降脂药物靶点与36种循环炎症细胞因子的直接因果关系。最后,对已确定的细胞因子进行富集分析,以探讨降脂药物与炎症反应的潜在关系。
结果
基因代理的胆固醇酯转运蛋白(CETP)抑制剂与脓毒症相关重症监护入院显著相关(比值比=0.84,95%置信区间[0.74,0.95],P=0.008)和脓毒症相关死亡(比值比=0.68,95%置信区间[0.52,0.88],P=0.004)。基因代理的CETP抑制剂与15种循环炎症细胞因子的水平密切相关。富集分析表明,CETP抑制剂可能调节炎症细胞因子并影响炎症反应途径。
结论
本研究支持基因代理的CETP抑制剂在降低脓毒症相关重症监护入院和死亡风险方面的因果效应。这些发现表明,潜在机制可能涉及对一些循环炎症细胞因子的调节,影响炎症反应途径。
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