Modulation of Metabolomic Profile in Sepsis According to the State of Immune Activation.

IF 7.7 1区 医学 Q1 CRITICAL CARE MEDICINE Critical Care Medicine Pub Date : 2024-11-01 Epub Date: 2024-08-23 DOI:10.1097/CCM.0000000000006391
Eleftheria Kranidioti, Isis Ricaño-Ponce, Nikolaos Antonakos, Evdoxia Kyriazopoulou, Antigone Kotsaki, Iraklis Tsangaris, Dimitra Markopoulou, Nikoleta Rovina, Eleni Antoniadou, Ioannis Koutsodimitropoulos, George N Dalekos, Glykeria Vlachogianni, Karolina Akinosoglou, Vasilios Koulouras, Apostolos Komnos, Theano Kontopoulou, George Dimopoulos, Mihai G Netea, Vinod Kumar, Evangelos J Giamarellos-Bourboulis
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Abstract

Objective: To investigate the metabolomic profiles associated with different immune activation states in sepsis patients.

Design: Subgroup analysis of the PROVIDE (a Personalized Randomized trial of Validation and restoration of Immune Dysfunction in severe infections and Sepsis) prospective clinical study.

Setting: Results of the PROVIDE study showed that patients with sepsis may be classified into three states of immune activation: 1) macrophage-activation-like syndrome (MALS) characterized by hyperinflammation, sepsis-induced immunoparalysis, and 3) unclassified or intermediate patients without severe immune dysregulation.

Patients or subjects: Two hundred ten patients from 14 clinical sites in Greece meeting the Sepsis-3 definitions with lung infection, acute cholangitis, or primary bacteremia.

Interventions: During our comparison, we did not perform any intervention.

Measurements and main results: Untargeted metabolomics analysis was performed on plasma samples from 210 patients (a total of 1394 products). Differential abundance analysis identified 221 significantly different metabolites across the immune states. Metabolites were enriched in pathways related to ubiquinone biosynthesis, tyrosine metabolism, and tryptophan metabolism when comparing MALS to immunoparalysis and unclassified patients. When comparing MALS to unclassified, 312 significantly different metabolites were found, and pathway analysis indicated enrichment in multiple pathways. Comparing immunoparalysis to unclassified patients revealed only two differentially regulated metabolites.

Conclusions: Findings suggest distinct metabolic dysregulation patterns associated with different immune dysfunctions in sepsis: the strongest metabolic dysregulation is associated with MALS.

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根据免疫激活状态调节败血症的代谢组谱
目的研究与败血症患者不同免疫激活状态相关的代谢组学特征:PROVIDE(重症感染和脓毒症免疫功能失调的验证和恢复的个性化随机试验)前瞻性临床研究的分组分析:PROVIDE研究结果显示,败血症患者可分为三种免疫激活状态:1)以炎症亢进为特征的巨噬细胞活化样综合征(MALS);2)脓毒症诱发的免疫麻痹;3)未分类或无严重免疫失调的中间型患者:来自希腊 14 个临床机构的 210 名符合败血症-3 定义的肺部感染、急性胆管炎或原发性菌血症患者:在比较过程中,我们没有采取任何干预措施:对 210 名患者的血浆样本(共 1394 个产物)进行了非靶向代谢组学分析。差异丰度分析确定了221种在不同免疫状态下有显著差异的代谢物。当将 MALS 与免疫分析和未分类患者进行比较时,代谢物富集在与泛醌生物合成、酪氨酸代谢和色氨酸代谢相关的通路中。当将 MALS 与未分类患者进行比较时,发现有 312 种代谢物存在显著差异,而通路分析表明在多个通路中存在富集。将免疫分析法与未分类患者进行比较,发现只有两种代谢物受到不同的调控:结论:研究结果表明,脓毒症患者的代谢失调模式与不同的免疫功能障碍有关:最强的代谢失调与 MALS 有关。
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来源期刊
Critical Care Medicine
Critical Care Medicine 医学-危重病医学
CiteScore
16.30
自引率
5.70%
发文量
728
审稿时长
2 months
期刊介绍: Critical Care Medicine is the premier peer-reviewed, scientific publication in critical care medicine. Directed to those specialists who treat patients in the ICU and CCU, including chest physicians, surgeons, pediatricians, pharmacists/pharmacologists, anesthesiologists, critical care nurses, and other healthcare professionals, Critical Care Medicine covers all aspects of acute and emergency care for the critically ill or injured patient. Each issue presents critical care practitioners with clinical breakthroughs that lead to better patient care, the latest news on promising research, and advances in equipment and techniques.
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