Integrating Mendelian randomization and multi-omics analysis unravels gut microbiota-driven metabolic mechanisms in sepsis and identifies diagnostic biomarkers through experimental validation
Guangyao Wang, Yuanyuan Liu, Jinjing Tan, Liqun Li, Jing Yan, Jing Liang, Xiaohua Hong, Sheng Xie

TL;DR
This study combines genetic and multi-omics data to uncover how gut microbes like Prevotella 9 influence sepsis through fatty acid metabolism and identifies potential biomarkers for diagnosis.
Contribution
Novel integration of Mendelian randomization and multi-omics data to identify causal gut microbiota-metabolite interactions and validate diagnostic biomarkers in sepsis.
Findings
Prevotella 9 shows protective effects in sepsis through regulation of fatty acid metabolism.
Three key diagnostic genes (ABCC1, CYP1B1, PPARG) are identified and validated for sepsis.
Monocytes are highlighted as potential cellular targets in sepsis via immunometabolic pathways.
Abstract
Sepsis, a life-threatening systemic inflammatory syndrome, remains a leading cause of global mortality due to its complex pathophysiology and the lack of specific diagnostic biomarkers. Recent evidence highlights intricate interactions between the gut microbiota, metabolites, and host inflammatory responses; however, the causal relationships and underlying mechanisms remain poorly understood. We integrated Mendelian randomization (MR) with multi-omics approaches (including transcriptomics, untargeted metabolomics, and single-cell transcriptomics) to elucidate the causal relationships and underlying mechanisms between gut microbiota and their associated metabolites in the inflammatory response of sepsis. Building on this analysis, we employed machine learning algorithms to identify sepsis-specific diagnostic biomarkers derived from Prevotella 9, fatty acids, and PANoptosis-related genes.…
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Taxonomy
TopicsGut microbiota and health · Sepsis Diagnosis and Treatment · Immune Response and Inflammation
