%0 Journal Article %T Clinical features and multiomics profiles indicate coagulation and platelet dysfunction in COVID-19 viral sepsis. %A Xiao Z %A Lin M %A Song N %A Wu X %A Hou J %A Wang L %A Tian X %A An C %A Dela Cruz CS %A Sharma L %A Chang %J iScience %V 27 %N 6 %D 2024 Jun 21 %M 38974472 %F 6.107 %R 10.1016/j.isci.2024.110110 %X Increased cases of sepsis during COVID-19 in the absence of known bacterial pathogens highlighted role of viruses as causative agents of sepsis. In this study, we investigated clinical, laboratory, proteomic, and metabolomic characteristics of viral sepsis patients (n = 45) and compared them to non-sepsis patients with COVID-19 (n = 186) to identify molecular mechanisms underlying the pathology of viral sepsis in COVID-19. We identified unique metabolomic and proteomic signatures that suggest a substantial perturbation in the coagulation, complement, and platelet activation pathways in viral sepsis. Our proteomic data indicated elevated coagulation pathway protein (fibrinogen), whereas a decrease in many of the complement proteins was observed. These alterations were associated with the functional consequences such as susceptibility to secondary bacterial infections and potentially contributing to both local and systemic disease phenotypes. Our data provide novel aspect of COVID-19 pathology that is centered around presence of sepsis phenotype in COVID-19.