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The prognostic impact of SIGLEC5-induced impairment of CD8(+) T cell activation in sepsis

BACKGROUND: Sepsis is associated with T-cell exhaustion, which significantly reduces patient outcomes. Therefore, targeting of immune checkpoints (ICs) is deemed necessary for effective sepsis management. Here, we evaluated the role of SIGLEC5 as an IC ligand and explored its potential as a biomarke...

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Autores principales: Lozano-Rodríguez, Roberto, Avendaño-Ortíz, José, Montalbán-Hernández, Karla, Ruiz-Rodríguez, Juan Carlos, Ferrer, Ricardo, Martín-Quirós, Alejandro, Maroun-Eid, Charbel, González-López, Juan José, Fàbrega, Anna, Terrón-Arcos, Verónica, Gutiérrez-Fernández, María, Alonso-López, Elisa, Cubillos-Zapata, Carolina, Fernández-Velasco, María, Pérez de Diego, Rebeca, Pelegrin, Pablo, García-Palenciano, Carlos, Cueto, Francisco J., del Fresno, Carlos, López-Collazo, Eduardo
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Elsevier 2023
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10630607/
https://www.ncbi.nlm.nih.gov/pubmed/37890368
http://dx.doi.org/10.1016/j.ebiom.2023.104841
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author Lozano-Rodríguez, Roberto
Avendaño-Ortíz, José
Montalbán-Hernández, Karla
Ruiz-Rodríguez, Juan Carlos
Ferrer, Ricardo
Martín-Quirós, Alejandro
Maroun-Eid, Charbel
González-López, Juan José
Fàbrega, Anna
Terrón-Arcos, Verónica
Gutiérrez-Fernández, María
Alonso-López, Elisa
Cubillos-Zapata, Carolina
Fernández-Velasco, María
Pérez de Diego, Rebeca
Pelegrin, Pablo
García-Palenciano, Carlos
Cueto, Francisco J.
del Fresno, Carlos
López-Collazo, Eduardo
author_facet Lozano-Rodríguez, Roberto
Avendaño-Ortíz, José
Montalbán-Hernández, Karla
Ruiz-Rodríguez, Juan Carlos
Ferrer, Ricardo
Martín-Quirós, Alejandro
Maroun-Eid, Charbel
González-López, Juan José
Fàbrega, Anna
Terrón-Arcos, Verónica
Gutiérrez-Fernández, María
Alonso-López, Elisa
Cubillos-Zapata, Carolina
Fernández-Velasco, María
Pérez de Diego, Rebeca
Pelegrin, Pablo
García-Palenciano, Carlos
Cueto, Francisco J.
del Fresno, Carlos
López-Collazo, Eduardo
author_sort Lozano-Rodríguez, Roberto
collection PubMed
description BACKGROUND: Sepsis is associated with T-cell exhaustion, which significantly reduces patient outcomes. Therefore, targeting of immune checkpoints (ICs) is deemed necessary for effective sepsis management. Here, we evaluated the role of SIGLEC5 as an IC ligand and explored its potential as a biomarker for sepsis. METHODS: In vitro and in vivo assays were conducted to both analyse SIGLEC5's role as an IC ligand, as well as assess its impact on survival in sepsis. A multicentre prospective cohort study was conducted to evaluate the plasmatic soluble SIGLEC5 (sSIGLEC5) as a mortality predictor in the first 60 days after admission in sepsis patients. Recruitment included sepsis patients (n = 346), controls with systemic inflammatory response syndrome (n = 80), aneurism (n = 11), stroke (n = 16), and healthy volunteers (HVs, n = 100). FINDINGS: SIGLEC5 expression on monocytes was increased by HIF1α and was higher in septic patients than in healthy volunteers after ex vivo LPS challenge. Furthermore, SIGLEC5-PSGL1 interaction inhibited CD8(+) T-cell proliferation. Administration of sSIGLEC5r (0.8 mg/kg) had adverse effects in mouse endotoxemia models. Additionally, plasma sSIGLEC5 levels of septic patients were higher than HVs and ROC analysis revealed it as a mortality marker with an AUC of 0.713 (95% CI, 0.656–0.769; p < 0.0001). Kaplan–Meier survival curve showed a significant decrease in survival above the calculated cut-off (HR of 3.418, 95% CI, 2.380–4.907, p < 0.0001 by log-rank test) estimated by Youden Index (523.6 ng/mL). INTERPRETATION: SIGLEC5 displays the hallmarks of an IC ligand, and plasma levels of sSIGLEC5 have been linked with increased mortality in septic patients. FUNDING: 10.13039/501100004587Instituto de Salud Carlos III (ISCIII) and “Fondos FEDER” to 10.13039/100006520ELC (PIE15/00065, PI18/00148, PI14/01234, PI21/00869), 10.13039/100002768CDF (PI21/01178), RLR (FI19/00334) and JAO (CD21/00059).
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spelling pubmed-106306072023-10-25 The prognostic impact of SIGLEC5-induced impairment of CD8(+) T cell activation in sepsis Lozano-Rodríguez, Roberto Avendaño-Ortíz, José Montalbán-Hernández, Karla Ruiz-Rodríguez, Juan Carlos Ferrer, Ricardo Martín-Quirós, Alejandro Maroun-Eid, Charbel González-López, Juan José Fàbrega, Anna Terrón-Arcos, Verónica Gutiérrez-Fernández, María Alonso-López, Elisa Cubillos-Zapata, Carolina Fernández-Velasco, María Pérez de Diego, Rebeca Pelegrin, Pablo García-Palenciano, Carlos Cueto, Francisco J. del Fresno, Carlos López-Collazo, Eduardo eBioMedicine Articles BACKGROUND: Sepsis is associated with T-cell exhaustion, which significantly reduces patient outcomes. Therefore, targeting of immune checkpoints (ICs) is deemed necessary for effective sepsis management. Here, we evaluated the role of SIGLEC5 as an IC ligand and explored its potential as a biomarker for sepsis. METHODS: In vitro and in vivo assays were conducted to both analyse SIGLEC5's role as an IC ligand, as well as assess its impact on survival in sepsis. A multicentre prospective cohort study was conducted to evaluate the plasmatic soluble SIGLEC5 (sSIGLEC5) as a mortality predictor in the first 60 days after admission in sepsis patients. Recruitment included sepsis patients (n = 346), controls with systemic inflammatory response syndrome (n = 80), aneurism (n = 11), stroke (n = 16), and healthy volunteers (HVs, n = 100). FINDINGS: SIGLEC5 expression on monocytes was increased by HIF1α and was higher in septic patients than in healthy volunteers after ex vivo LPS challenge. Furthermore, SIGLEC5-PSGL1 interaction inhibited CD8(+) T-cell proliferation. Administration of sSIGLEC5r (0.8 mg/kg) had adverse effects in mouse endotoxemia models. Additionally, plasma sSIGLEC5 levels of septic patients were higher than HVs and ROC analysis revealed it as a mortality marker with an AUC of 0.713 (95% CI, 0.656–0.769; p < 0.0001). Kaplan–Meier survival curve showed a significant decrease in survival above the calculated cut-off (HR of 3.418, 95% CI, 2.380–4.907, p < 0.0001 by log-rank test) estimated by Youden Index (523.6 ng/mL). INTERPRETATION: SIGLEC5 displays the hallmarks of an IC ligand, and plasma levels of sSIGLEC5 have been linked with increased mortality in septic patients. FUNDING: 10.13039/501100004587Instituto de Salud Carlos III (ISCIII) and “Fondos FEDER” to 10.13039/100006520ELC (PIE15/00065, PI18/00148, PI14/01234, PI21/00869), 10.13039/100002768CDF (PI21/01178), RLR (FI19/00334) and JAO (CD21/00059). Elsevier 2023-10-25 /pmc/articles/PMC10630607/ /pubmed/37890368 http://dx.doi.org/10.1016/j.ebiom.2023.104841 Text en © 2023 The Author(s) https://creativecommons.org/licenses/by-nc-nd/4.0/This is an open access article under the CC BY-NC-ND license (http://creativecommons.org/licenses/by-nc-nd/4.0/).
spellingShingle Articles
Lozano-Rodríguez, Roberto
Avendaño-Ortíz, José
Montalbán-Hernández, Karla
Ruiz-Rodríguez, Juan Carlos
Ferrer, Ricardo
Martín-Quirós, Alejandro
Maroun-Eid, Charbel
González-López, Juan José
Fàbrega, Anna
Terrón-Arcos, Verónica
Gutiérrez-Fernández, María
Alonso-López, Elisa
Cubillos-Zapata, Carolina
Fernández-Velasco, María
Pérez de Diego, Rebeca
Pelegrin, Pablo
García-Palenciano, Carlos
Cueto, Francisco J.
del Fresno, Carlos
López-Collazo, Eduardo
The prognostic impact of SIGLEC5-induced impairment of CD8(+) T cell activation in sepsis
title The prognostic impact of SIGLEC5-induced impairment of CD8(+) T cell activation in sepsis
title_full The prognostic impact of SIGLEC5-induced impairment of CD8(+) T cell activation in sepsis
title_fullStr The prognostic impact of SIGLEC5-induced impairment of CD8(+) T cell activation in sepsis
title_full_unstemmed The prognostic impact of SIGLEC5-induced impairment of CD8(+) T cell activation in sepsis
title_short The prognostic impact of SIGLEC5-induced impairment of CD8(+) T cell activation in sepsis
title_sort prognostic impact of siglec5-induced impairment of cd8(+) t cell activation in sepsis
topic Articles
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10630607/
https://www.ncbi.nlm.nih.gov/pubmed/37890368
http://dx.doi.org/10.1016/j.ebiom.2023.104841
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