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Identificador persistente para citar o vincular este elemento: https://accedacris.ulpgc.es/jspui/handle/10553/163118
Título: Acyl-CoA-binding protein (ACBP): a poor-prognosis biomarker in sepsis and a target for disease mitigation
Autores/as: Lambertucci, Flavia
Motino, Omar
Nogueira-Recalde, Uxia
Rong, Yan
Montegut, Lea
Perez-Lanzon, Maria
Carbonnier, Vincent
Li, Sijing
Durand, Sylvere
Aprahamian, Fanny
Chen, Hui
Dong, Yanbing
Sauvat, Allan
Mingoia, Silvia
Lachkar, Sylvie
Saavedra Díaz,Ester Gloria 
Pol, Jonathan
Pietrocola, Federico
Maiuri, Maria Chiara
Rocha-Oliveira, Estela
Roncon-Albuquerque, Roberto
Vasques-Novoa, Francisco
Lozano-Rodriguez, Roberto
Avendano-Ortiz, Jose
Lopez-Collazo, Eduardo
Abdellatif, Mahmoud
Martins, Isabelle
Kroemer, Guido
Clasificación UNESCO: 32 Ciencias médicas
3201 Ciencias clínicas
Palabras clave: Gaba(A) Receptors
Septic Shock
Bone-Marrow
Diazepam
Neutrophils, et al.
Fecha de publicación: 2025
Publicación seriada: Signal Transduction and Targeted Therapy 
Resumen: Sepsis remains a major clinical challenge, with high mortality and long-term disability despite current interventions. Here, we identify the tissue hormone acyl-CoA-binding protein (ACBP), also known as diazepam-binding inhibitor (DBI), as a biomarker and driver of poor outcome in sepsis. ACBP/DBI was elevated in the plasma of septic patients and associated with organ dysfunction and increased mortality. In murine models of endotoxemia, Escherichia coli infection, and polymicrobial sepsis, genetic deletion or antibody-mediated neutralization of ACBP/DBI conferred robust protection by dampening cytokine storm and preserving organ function. Across these three models, neutralization of ACBP/DBI with monoclonal antibodies restored thermoregulation and reduced mortality. Mechanistically, ACBP/DBI inhibition enhanced resilience to lipopolysaccharide-induced sterile inflammation and improved bacterial clearance by macrophages and granulocytes in vivo and in vitro. These effects were observed in monomicrobial infection models and confirmed by high-dimensional immunophenotyping in a polymicrobial sepsis model. Notably, ACBP/DBI inhibition could be favorably combined with glucocorticoids, enhancing survival and reversing histopathological, transcriptional or metabolic signatures of septic shock across heart, kidney, liver, lung, spleen and plasma. These findings position ACBP/DBI as a mechanistic amplifier of sepsis pathophysiology and propose its neutralization, alone or in combination with corticosteroids, as a promising therapeutic strategy to interrupt the fatal trajectory of septic shock.
URI: https://accedacris.ulpgc.es/jspui/handle/10553/163118
ISSN: 2095-9907
DOI: 10.1038/s41392-026-02670-z
Fuente: Signal Transduction And Targeted Therapy[ISSN 2095-9907],v. 11 (1), (Abril 2026)
Colección:Artículos
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