Fragile neutrophils in surgical patients: A phenomenon associated with critical illness

Leukocyte viability (determined by e.g. propidium iodide [PI] staining) is automatically measured by hematology analyzers to check for delayed bench time. Incidental findings in fresh blood samples revealed the existence of leukocytes with decreased viability in critically ill surgical patients. Not...

Descripción completa

Detalles Bibliográficos
Autores principales: Hesselink, Lillian, Spijkerman, Roy, Hellebrekers, Pien, van Bourgondiën, Robert J., Blasse, Enja, Haitjema, Saskia, Huisman, Albert, van Solinge, Wouter W., Van Wessem, Karlijn J. P., Koenderman, Leo, Leenen, Luke P. H., Hietbrink, Falco
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2020
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7402494/
https://www.ncbi.nlm.nih.gov/pubmed/32750099
http://dx.doi.org/10.1371/journal.pone.0236596
_version_ 1783566767811985408
author Hesselink, Lillian
Spijkerman, Roy
Hellebrekers, Pien
van Bourgondiën, Robert J.
Blasse, Enja
Haitjema, Saskia
Huisman, Albert
van Solinge, Wouter W.
Van Wessem, Karlijn J. P.
Koenderman, Leo
Leenen, Luke P. H.
Hietbrink, Falco
author_facet Hesselink, Lillian
Spijkerman, Roy
Hellebrekers, Pien
van Bourgondiën, Robert J.
Blasse, Enja
Haitjema, Saskia
Huisman, Albert
van Solinge, Wouter W.
Van Wessem, Karlijn J. P.
Koenderman, Leo
Leenen, Luke P. H.
Hietbrink, Falco
author_sort Hesselink, Lillian
collection PubMed
description Leukocyte viability (determined by e.g. propidium iodide [PI] staining) is automatically measured by hematology analyzers to check for delayed bench time. Incidental findings in fresh blood samples revealed the existence of leukocytes with decreased viability in critically ill surgical patients. Not much is known about these cells and their functional and/or clinical implications. Therefore, we investigated the incidence of decreased leukocyte viability, the implications for leukocyte functioning and its relation with clinical outcomes. An automated alarm was set in a routine hematology analyzer (Cell-Dyn Sapphire) for the presence of non-viable leukocytes characterized by increased fluorescence in the PI-channel (FL3:630±30nm). Patients with non-viable leukocytes were prospectively included and blood samples were drawn to investigate leukocyte viability in detail and to investigate leukocyte functioning (phagocytosis and responsiveness to a bacterial stimulus). Then, a retrospective analysis was conducted to investigate the incidence of fragile neutrophils in the circulation and clinical outcomes of surgical patients with fragile neutrophils hospitalized between 2013–2017. A high FL3 signal was either caused by 1) neutrophil autofluorescence which was considered false positive, or by 2) actual non-viable PI-positive neutrophils in the blood sample. These two causes could be distinguished using automatically generated data from the hematology analyzer. The non-viable (PI-positive) neutrophils proved to be viable (PI-negative) in non-lysed blood samples, and were therefore referred to as ‘fragile neutrophils’. Overall leukocyte functioning was not impaired in patients with fragile neutrophils. Of the 11 872 retrospectively included surgical patients, 75 (0.63%) were identified to have fragile neutrophils during hospitalization. Of all patients with fragile neutrophils, 75.7% developed an infection, 70.3% were admitted to the ICU and 31.3% died during hospitalization. In conclusion, fragile neutrophils occur in the circulation of critically ill surgical patients. These cells can be automatically detected during routine blood analyses and are an indicator of critical illness.
format Online
Article
Text
id pubmed-7402494
institution National Center for Biotechnology Information
language English
publishDate 2020
publisher Public Library of Science
record_format MEDLINE/PubMed
spelling pubmed-74024942020-08-12 Fragile neutrophils in surgical patients: A phenomenon associated with critical illness Hesselink, Lillian Spijkerman, Roy Hellebrekers, Pien van Bourgondiën, Robert J. Blasse, Enja Haitjema, Saskia Huisman, Albert van Solinge, Wouter W. Van Wessem, Karlijn J. P. Koenderman, Leo Leenen, Luke P. H. Hietbrink, Falco PLoS One Research Article Leukocyte viability (determined by e.g. propidium iodide [PI] staining) is automatically measured by hematology analyzers to check for delayed bench time. Incidental findings in fresh blood samples revealed the existence of leukocytes with decreased viability in critically ill surgical patients. Not much is known about these cells and their functional and/or clinical implications. Therefore, we investigated the incidence of decreased leukocyte viability, the implications for leukocyte functioning and its relation with clinical outcomes. An automated alarm was set in a routine hematology analyzer (Cell-Dyn Sapphire) for the presence of non-viable leukocytes characterized by increased fluorescence in the PI-channel (FL3:630±30nm). Patients with non-viable leukocytes were prospectively included and blood samples were drawn to investigate leukocyte viability in detail and to investigate leukocyte functioning (phagocytosis and responsiveness to a bacterial stimulus). Then, a retrospective analysis was conducted to investigate the incidence of fragile neutrophils in the circulation and clinical outcomes of surgical patients with fragile neutrophils hospitalized between 2013–2017. A high FL3 signal was either caused by 1) neutrophil autofluorescence which was considered false positive, or by 2) actual non-viable PI-positive neutrophils in the blood sample. These two causes could be distinguished using automatically generated data from the hematology analyzer. The non-viable (PI-positive) neutrophils proved to be viable (PI-negative) in non-lysed blood samples, and were therefore referred to as ‘fragile neutrophils’. Overall leukocyte functioning was not impaired in patients with fragile neutrophils. Of the 11 872 retrospectively included surgical patients, 75 (0.63%) were identified to have fragile neutrophils during hospitalization. Of all patients with fragile neutrophils, 75.7% developed an infection, 70.3% were admitted to the ICU and 31.3% died during hospitalization. In conclusion, fragile neutrophils occur in the circulation of critically ill surgical patients. These cells can be automatically detected during routine blood analyses and are an indicator of critical illness. Public Library of Science 2020-08-04 /pmc/articles/PMC7402494/ /pubmed/32750099 http://dx.doi.org/10.1371/journal.pone.0236596 Text en © 2020 Hesselink et al http://creativecommons.org/licenses/by/4.0/ This is an open access article distributed under the terms of the Creative Commons Attribution License (http://creativecommons.org/licenses/by/4.0/) , which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited.
spellingShingle Research Article
Hesselink, Lillian
Spijkerman, Roy
Hellebrekers, Pien
van Bourgondiën, Robert J.
Blasse, Enja
Haitjema, Saskia
Huisman, Albert
van Solinge, Wouter W.
Van Wessem, Karlijn J. P.
Koenderman, Leo
Leenen, Luke P. H.
Hietbrink, Falco
Fragile neutrophils in surgical patients: A phenomenon associated with critical illness
title Fragile neutrophils in surgical patients: A phenomenon associated with critical illness
title_full Fragile neutrophils in surgical patients: A phenomenon associated with critical illness
title_fullStr Fragile neutrophils in surgical patients: A phenomenon associated with critical illness
title_full_unstemmed Fragile neutrophils in surgical patients: A phenomenon associated with critical illness
title_short Fragile neutrophils in surgical patients: A phenomenon associated with critical illness
title_sort fragile neutrophils in surgical patients: a phenomenon associated with critical illness
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7402494/
https://www.ncbi.nlm.nih.gov/pubmed/32750099
http://dx.doi.org/10.1371/journal.pone.0236596
work_keys_str_mv AT hesselinklillian fragileneutrophilsinsurgicalpatientsaphenomenonassociatedwithcriticalillness
AT spijkermanroy fragileneutrophilsinsurgicalpatientsaphenomenonassociatedwithcriticalillness
AT hellebrekerspien fragileneutrophilsinsurgicalpatientsaphenomenonassociatedwithcriticalillness
AT vanbourgondienrobertj fragileneutrophilsinsurgicalpatientsaphenomenonassociatedwithcriticalillness
AT blasseenja fragileneutrophilsinsurgicalpatientsaphenomenonassociatedwithcriticalillness
AT haitjemasaskia fragileneutrophilsinsurgicalpatientsaphenomenonassociatedwithcriticalillness
AT huismanalbert fragileneutrophilsinsurgicalpatientsaphenomenonassociatedwithcriticalillness
AT vansolingewouterw fragileneutrophilsinsurgicalpatientsaphenomenonassociatedwithcriticalillness
AT vanwessemkarlijnjp fragileneutrophilsinsurgicalpatientsaphenomenonassociatedwithcriticalillness
AT koendermanleo fragileneutrophilsinsurgicalpatientsaphenomenonassociatedwithcriticalillness
AT leenenlukeph fragileneutrophilsinsurgicalpatientsaphenomenonassociatedwithcriticalillness
AT hietbrinkfalco fragileneutrophilsinsurgicalpatientsaphenomenonassociatedwithcriticalillness

Ejemplares similares