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Elevated Admission Base Deficit Is Associated with a Complex Dynamic Network of Systemic Inflammation Which Drives Clinical Trajectories in Blunt Trauma Patients

We hypothesized that elevated base deficit (BD) ≥ 4 mEq/L upon admission could be associated with an altered inflammatory response, which in turn may impact differential clinical trajectories. Using clinical and biobank data from 472 blunt trauma survivors, 154 patients were identified after excludi...

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Autores principales: Abdul-Malak, Othman, Vodovotz, Yoram, Zaaqoq, Akram, Guardado, Jesse, Almahmoud, Khalid, Yin, Jinling, Zuckerbraun, Brian, Peitzman, Andrew B., Sperry, Jason, Billiar, Timothy R., Namas, Rami A.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Hindawi Publishing Corporation 2016
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5126463/
https://www.ncbi.nlm.nih.gov/pubmed/27974867
http://dx.doi.org/10.1155/2016/7950374
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author Abdul-Malak, Othman
Vodovotz, Yoram
Zaaqoq, Akram
Guardado, Jesse
Almahmoud, Khalid
Yin, Jinling
Zuckerbraun, Brian
Peitzman, Andrew B.
Sperry, Jason
Billiar, Timothy R.
Namas, Rami A.
author_facet Abdul-Malak, Othman
Vodovotz, Yoram
Zaaqoq, Akram
Guardado, Jesse
Almahmoud, Khalid
Yin, Jinling
Zuckerbraun, Brian
Peitzman, Andrew B.
Sperry, Jason
Billiar, Timothy R.
Namas, Rami A.
author_sort Abdul-Malak, Othman
collection PubMed
description We hypothesized that elevated base deficit (BD) ≥ 4 mEq/L upon admission could be associated with an altered inflammatory response, which in turn may impact differential clinical trajectories. Using clinical and biobank data from 472 blunt trauma survivors, 154 patients were identified after excluding patients who received prehospital IV fluids or had alcohol intoxication. From this subcohort, 84 patients had a BD ≥ 4 mEq/L and 70 patients with BD < 4 mEq/L. Three samples within the first 24 h were obtained from all patients and then daily up to day 7 after injury. Twenty-two cytokines and chemokines were assayed using Luminex™ and were analyzed using two-way ANOVA and dynamic network analysis (DyNA). Multiple mediators of the innate and lymphoid immune responses in the BD ≥ 4 group were elevated differentially upon admission and up to 16 h after injury. DyNA revealed a higher, sustained degree of interconnectivity of the inflammatory response in the BD ≥ 4 patients during the initial 16 h after injury. These results suggest that elevated admission BD is associated with differential immune/inflammatory pathways, which subsequently could predispose patients to follow a complicated clinical course.
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spelling pubmed-51264632016-12-14 Elevated Admission Base Deficit Is Associated with a Complex Dynamic Network of Systemic Inflammation Which Drives Clinical Trajectories in Blunt Trauma Patients Abdul-Malak, Othman Vodovotz, Yoram Zaaqoq, Akram Guardado, Jesse Almahmoud, Khalid Yin, Jinling Zuckerbraun, Brian Peitzman, Andrew B. Sperry, Jason Billiar, Timothy R. Namas, Rami A. Mediators Inflamm Research Article We hypothesized that elevated base deficit (BD) ≥ 4 mEq/L upon admission could be associated with an altered inflammatory response, which in turn may impact differential clinical trajectories. Using clinical and biobank data from 472 blunt trauma survivors, 154 patients were identified after excluding patients who received prehospital IV fluids or had alcohol intoxication. From this subcohort, 84 patients had a BD ≥ 4 mEq/L and 70 patients with BD < 4 mEq/L. Three samples within the first 24 h were obtained from all patients and then daily up to day 7 after injury. Twenty-two cytokines and chemokines were assayed using Luminex™ and were analyzed using two-way ANOVA and dynamic network analysis (DyNA). Multiple mediators of the innate and lymphoid immune responses in the BD ≥ 4 group were elevated differentially upon admission and up to 16 h after injury. DyNA revealed a higher, sustained degree of interconnectivity of the inflammatory response in the BD ≥ 4 patients during the initial 16 h after injury. These results suggest that elevated admission BD is associated with differential immune/inflammatory pathways, which subsequently could predispose patients to follow a complicated clinical course. Hindawi Publishing Corporation 2016 2016-11-15 /pmc/articles/PMC5126463/ /pubmed/27974867 http://dx.doi.org/10.1155/2016/7950374 Text en Copyright © 2016 Othman Abdul-Malak et al. https://creativecommons.org/licenses/by/4.0/ This is an open access article distributed under the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original work is properly cited.
spellingShingle Research Article
Abdul-Malak, Othman
Vodovotz, Yoram
Zaaqoq, Akram
Guardado, Jesse
Almahmoud, Khalid
Yin, Jinling
Zuckerbraun, Brian
Peitzman, Andrew B.
Sperry, Jason
Billiar, Timothy R.
Namas, Rami A.
Elevated Admission Base Deficit Is Associated with a Complex Dynamic Network of Systemic Inflammation Which Drives Clinical Trajectories in Blunt Trauma Patients
title Elevated Admission Base Deficit Is Associated with a Complex Dynamic Network of Systemic Inflammation Which Drives Clinical Trajectories in Blunt Trauma Patients
title_full Elevated Admission Base Deficit Is Associated with a Complex Dynamic Network of Systemic Inflammation Which Drives Clinical Trajectories in Blunt Trauma Patients
title_fullStr Elevated Admission Base Deficit Is Associated with a Complex Dynamic Network of Systemic Inflammation Which Drives Clinical Trajectories in Blunt Trauma Patients
title_full_unstemmed Elevated Admission Base Deficit Is Associated with a Complex Dynamic Network of Systemic Inflammation Which Drives Clinical Trajectories in Blunt Trauma Patients
title_short Elevated Admission Base Deficit Is Associated with a Complex Dynamic Network of Systemic Inflammation Which Drives Clinical Trajectories in Blunt Trauma Patients
title_sort elevated admission base deficit is associated with a complex dynamic network of systemic inflammation which drives clinical trajectories in blunt trauma patients
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5126463/
https://www.ncbi.nlm.nih.gov/pubmed/27974867
http://dx.doi.org/10.1155/2016/7950374
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