A Pilot Study on Continuous Infusion of 4% Albumin in Critically Ill Patients: Impact on Nosocomial Infection via a Reduction Mechanism for Oxidized Substrates

Care-related infections affect up to 11% of ICU patients. Running therapeutic albumin is sometimes associated to less infection: whether a specific method of its infusion is of any interest to modulate innate defense is unknown. Our objectives were: 1) to test whether the method for albumin infusion...

Descripción completa

Detalles Bibliográficos
Autores principales: Schneider, Francis, Dureau, Anne-Florence, Hellé, Sophie, Betscha, Cosette, Senger, Bernard, Cremel, Gérard, Boulmedais, Fouzia, Strub, Jean-Marc, Corti, Angelo, Meyer, Nicolas, Guillot, Max, Schaaf, Pierre, Metz-Boutigue, Marie-Hélène
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Wolters Kluwer Health 2019
Materias:
Original Clinical Report
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7063941/
https://www.ncbi.nlm.nih.gov/pubmed/32166286
http://dx.doi.org/10.1097/CCE.0000000000000044
_version_ 1783504786333630464
author Schneider, Francis
Dureau, Anne-Florence
Hellé, Sophie
Betscha, Cosette
Senger, Bernard
Cremel, Gérard
Boulmedais, Fouzia
Strub, Jean-Marc
Corti, Angelo
Meyer, Nicolas
Guillot, Max
Schaaf, Pierre
Metz-Boutigue, Marie-Hélène
author_facet Schneider, Francis
Dureau, Anne-Florence
Hellé, Sophie
Betscha, Cosette
Senger, Bernard
Cremel, Gérard
Boulmedais, Fouzia
Strub, Jean-Marc
Corti, Angelo
Meyer, Nicolas
Guillot, Max
Schaaf, Pierre
Metz-Boutigue, Marie-Hélène
author_sort Schneider, Francis
collection PubMed
description Care-related infections affect up to 11% of ICU patients. Running therapeutic albumin is sometimes associated to less infection: whether a specific method of its infusion is of any interest to modulate innate defense is unknown. Our objectives were: 1) to test whether the method for albumin infusion is important to prevent care-related infections and 2) to analyze in vitro the antioxidative role of albumin on host defense proteins during shock (using vasostatin-I as an example). DESIGN: In a prospective, randomized, open-label trial, shock patients were allocated to receive either continuously 4% albumin or intermittently 20% albumin, as long as they were infused with norepinephrine. A translational study including in vivo and in vitro analyses of albumin-vasostatin-I interactions is reported. SETTING: A tertiary ICU caring for 1,000 patients per year. PATIENTS: Fifty shock patients with serum albumin less than 20 g/L. INTERVENTIONS: In vivo colonization and nosocomial infections were recorded and time-dependent changes in serum albumin, chromogranin A, and vasostatin-I concentrations as well. In vitro, we studied biochemical albumin-vasostatin-I relationship using biochemical methods. MEASUREMENTS AND MAIN RESULTS: Over 18 days, we recorded a decrease in colonization (four vs 12 episodes; p = 0.035) and nosocomial infection frequency (two vs 13 episodes; p = 0.002) in patients infused continuously 4% albumin versus controls. In vitro, albumin interacts with the disulfide loop vasostatin-I (residues 17–40) and continuous 4% albumin infusion restores its oxidative status required for antimicrobial activity. CONCLUSIONS: Continuous 4% albumin is effective in reducing care-related infections in shock patients by increasing the availability of antimicrobial vasostatin-I. This might guide future care of shock patients.
format Online
Article
Text
id pubmed-7063941
institution National Center for Biotechnology Information
language English
publishDate 2019
publisher Wolters Kluwer Health
record_format MEDLINE/PubMed
spelling pubmed-70639412020-03-12 A Pilot Study on Continuous Infusion of 4% Albumin in Critically Ill Patients: Impact on Nosocomial Infection via a Reduction Mechanism for Oxidized Substrates Schneider, Francis Dureau, Anne-Florence Hellé, Sophie Betscha, Cosette Senger, Bernard Cremel, Gérard Boulmedais, Fouzia Strub, Jean-Marc Corti, Angelo Meyer, Nicolas Guillot, Max Schaaf, Pierre Metz-Boutigue, Marie-Hélène Crit Care Explor Original Clinical Report Care-related infections affect up to 11% of ICU patients. Running therapeutic albumin is sometimes associated to less infection: whether a specific method of its infusion is of any interest to modulate innate defense is unknown. Our objectives were: 1) to test whether the method for albumin infusion is important to prevent care-related infections and 2) to analyze in vitro the antioxidative role of albumin on host defense proteins during shock (using vasostatin-I as an example). DESIGN: In a prospective, randomized, open-label trial, shock patients were allocated to receive either continuously 4% albumin or intermittently 20% albumin, as long as they were infused with norepinephrine. A translational study including in vivo and in vitro analyses of albumin-vasostatin-I interactions is reported. SETTING: A tertiary ICU caring for 1,000 patients per year. PATIENTS: Fifty shock patients with serum albumin less than 20 g/L. INTERVENTIONS: In vivo colonization and nosocomial infections were recorded and time-dependent changes in serum albumin, chromogranin A, and vasostatin-I concentrations as well. In vitro, we studied biochemical albumin-vasostatin-I relationship using biochemical methods. MEASUREMENTS AND MAIN RESULTS: Over 18 days, we recorded a decrease in colonization (four vs 12 episodes; p = 0.035) and nosocomial infection frequency (two vs 13 episodes; p = 0.002) in patients infused continuously 4% albumin versus controls. In vitro, albumin interacts with the disulfide loop vasostatin-I (residues 17–40) and continuous 4% albumin infusion restores its oxidative status required for antimicrobial activity. CONCLUSIONS: Continuous 4% albumin is effective in reducing care-related infections in shock patients by increasing the availability of antimicrobial vasostatin-I. This might guide future care of shock patients. Wolters Kluwer Health 2019-09-19 /pmc/articles/PMC7063941/ /pubmed/32166286 http://dx.doi.org/10.1097/CCE.0000000000000044 Text en Copyright © 2019 The Authors. Published by Wolters Kluwer Health, Inc. on behalf of the Society of Critical Care Medicine. This is an open-access article distributed under the terms of the Creative Commons Attribution-Non Commercial-No Derivatives License 4.0 (CCBY-NC-ND) (http://creativecommons.org/licenses/by-nc-nd/4.0/) , where it is permissible to download and share the work provided it is properly cited. The work cannot be changed in any way or used commercially without permission from the journal.
spellingShingle Original Clinical Report
Schneider, Francis
Dureau, Anne-Florence
Hellé, Sophie
Betscha, Cosette
Senger, Bernard
Cremel, Gérard
Boulmedais, Fouzia
Strub, Jean-Marc
Corti, Angelo
Meyer, Nicolas
Guillot, Max
Schaaf, Pierre
Metz-Boutigue, Marie-Hélène
A Pilot Study on Continuous Infusion of 4% Albumin in Critically Ill Patients: Impact on Nosocomial Infection via a Reduction Mechanism for Oxidized Substrates
title A Pilot Study on Continuous Infusion of 4% Albumin in Critically Ill Patients: Impact on Nosocomial Infection via a Reduction Mechanism for Oxidized Substrates
title_full A Pilot Study on Continuous Infusion of 4% Albumin in Critically Ill Patients: Impact on Nosocomial Infection via a Reduction Mechanism for Oxidized Substrates
title_fullStr A Pilot Study on Continuous Infusion of 4% Albumin in Critically Ill Patients: Impact on Nosocomial Infection via a Reduction Mechanism for Oxidized Substrates
title_full_unstemmed A Pilot Study on Continuous Infusion of 4% Albumin in Critically Ill Patients: Impact on Nosocomial Infection via a Reduction Mechanism for Oxidized Substrates
title_short A Pilot Study on Continuous Infusion of 4% Albumin in Critically Ill Patients: Impact on Nosocomial Infection via a Reduction Mechanism for Oxidized Substrates
title_sort pilot study on continuous infusion of 4% albumin in critically ill patients: impact on nosocomial infection via a reduction mechanism for oxidized substrates
topic Original Clinical Report
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7063941/
https://www.ncbi.nlm.nih.gov/pubmed/32166286
http://dx.doi.org/10.1097/CCE.0000000000000044
work_keys_str_mv AT schneiderfrancis apilotstudyoncontinuousinfusionof4albuminincriticallyillpatientsimpactonnosocomialinfectionviaareductionmechanismforoxidizedsubstrates
AT dureauanneflorence apilotstudyoncontinuousinfusionof4albuminincriticallyillpatientsimpactonnosocomialinfectionviaareductionmechanismforoxidizedsubstrates
AT hellesophie apilotstudyoncontinuousinfusionof4albuminincriticallyillpatientsimpactonnosocomialinfectionviaareductionmechanismforoxidizedsubstrates
AT betschacosette apilotstudyoncontinuousinfusionof4albuminincriticallyillpatientsimpactonnosocomialinfectionviaareductionmechanismforoxidizedsubstrates
AT sengerbernard apilotstudyoncontinuousinfusionof4albuminincriticallyillpatientsimpactonnosocomialinfectionviaareductionmechanismforoxidizedsubstrates
AT cremelgerard apilotstudyoncontinuousinfusionof4albuminincriticallyillpatientsimpactonnosocomialinfectionviaareductionmechanismforoxidizedsubstrates
AT boulmedaisfouzia apilotstudyoncontinuousinfusionof4albuminincriticallyillpatientsimpactonnosocomialinfectionviaareductionmechanismforoxidizedsubstrates
AT strubjeanmarc apilotstudyoncontinuousinfusionof4albuminincriticallyillpatientsimpactonnosocomialinfectionviaareductionmechanismforoxidizedsubstrates
AT cortiangelo apilotstudyoncontinuousinfusionof4albuminincriticallyillpatientsimpactonnosocomialinfectionviaareductionmechanismforoxidizedsubstrates
AT meyernicolas apilotstudyoncontinuousinfusionof4albuminincriticallyillpatientsimpactonnosocomialinfectionviaareductionmechanismforoxidizedsubstrates
AT guillotmax apilotstudyoncontinuousinfusionof4albuminincriticallyillpatientsimpactonnosocomialinfectionviaareductionmechanismforoxidizedsubstrates
AT schaafpierre apilotstudyoncontinuousinfusionof4albuminincriticallyillpatientsimpactonnosocomialinfectionviaareductionmechanismforoxidizedsubstrates
AT metzboutiguemariehelene apilotstudyoncontinuousinfusionof4albuminincriticallyillpatientsimpactonnosocomialinfectionviaareductionmechanismforoxidizedsubstrates
AT schneiderfrancis pilotstudyoncontinuousinfusionof4albuminincriticallyillpatientsimpactonnosocomialinfectionviaareductionmechanismforoxidizedsubstrates
AT dureauanneflorence pilotstudyoncontinuousinfusionof4albuminincriticallyillpatientsimpactonnosocomialinfectionviaareductionmechanismforoxidizedsubstrates
AT hellesophie pilotstudyoncontinuousinfusionof4albuminincriticallyillpatientsimpactonnosocomialinfectionviaareductionmechanismforoxidizedsubstrates
AT betschacosette pilotstudyoncontinuousinfusionof4albuminincriticallyillpatientsimpactonnosocomialinfectionviaareductionmechanismforoxidizedsubstrates
AT sengerbernard pilotstudyoncontinuousinfusionof4albuminincriticallyillpatientsimpactonnosocomialinfectionviaareductionmechanismforoxidizedsubstrates
AT cremelgerard pilotstudyoncontinuousinfusionof4albuminincriticallyillpatientsimpactonnosocomialinfectionviaareductionmechanismforoxidizedsubstrates
AT boulmedaisfouzia pilotstudyoncontinuousinfusionof4albuminincriticallyillpatientsimpactonnosocomialinfectionviaareductionmechanismforoxidizedsubstrates
AT strubjeanmarc pilotstudyoncontinuousinfusionof4albuminincriticallyillpatientsimpactonnosocomialinfectionviaareductionmechanismforoxidizedsubstrates
AT cortiangelo pilotstudyoncontinuousinfusionof4albuminincriticallyillpatientsimpactonnosocomialinfectionviaareductionmechanismforoxidizedsubstrates
AT meyernicolas pilotstudyoncontinuousinfusionof4albuminincriticallyillpatientsimpactonnosocomialinfectionviaareductionmechanismforoxidizedsubstrates
AT guillotmax pilotstudyoncontinuousinfusionof4albuminincriticallyillpatientsimpactonnosocomialinfectionviaareductionmechanismforoxidizedsubstrates
AT schaafpierre pilotstudyoncontinuousinfusionof4albuminincriticallyillpatientsimpactonnosocomialinfectionviaareductionmechanismforoxidizedsubstrates
AT metzboutiguemariehelene pilotstudyoncontinuousinfusionof4albuminincriticallyillpatientsimpactonnosocomialinfectionviaareductionmechanismforoxidizedsubstrates

Ejemplares similares