Large-scale reduction of tyrosine kinase activities in human monocytes stimulated in vitro with N. meningitidis.

Large-scale reduction of tyrosine kinase activities in human monocytes stimulated in vitro with N. meningitidis.

N. meningitidis induces extensive gene expression changes in human monocytes, suggesting that complex networks of signaling pathways are activated during meningococcal sepsis. These effects are modulated by the anti-inflammatory cytokine interleukin-10 (IL-10). To further study changes in signal tra...

Full description

Bibliographic Details
Main Authors: Unni Gopinathan, Kathrine Røe Redalen, Anne-Marie Trøseid, Peter Kierulf, Petter Brandtzaeg, Anne Hansen Ree, Jens Petter Berg, Reidun Øvstebø
Format: Article
Language:English
Published: Public Library of Science (PLoS) 2018-01-01
Series:PLoS ONE
Online Access:http://europepmc.org/articles/PMC5774972?pdf=render
id doaj-61ce7492ad1644d793483765123c4d22
record_format Article
spelling doaj-61ce7492ad1644d793483765123c4d222020-11-25T01:22:08ZengPublic Library of Science (PLoS)PLoS ONE1932-62032018-01-01131e018191210.1371/journal.pone.0181912Large-scale reduction of tyrosine kinase activities in human monocytes stimulated in vitro with N. meningitidis.Unni GopinathanKathrine Røe RedalenAnne-Marie TrøseidPeter KierulfPetter BrandtzaegAnne Hansen ReeJens Petter BergReidun ØvstebøN. meningitidis induces extensive gene expression changes in human monocytes, suggesting that complex networks of signaling pathways are activated during meningococcal sepsis. These effects are modulated by the anti-inflammatory cytokine interleukin-10 (IL-10). To further study changes in signal transduction suggested by mRNA data, we used kinase substrate arrays to identify composite kinase activities induced by lysates from a primary human monocyte model system. Cell lysates were prepared from monocytes treated with the following experimental conditions: 106 N. meningitidis/mL, 25 ng/mL IL-10, 106 N. meningitidis/mL in combination with 25 ng/mL IL-10, and vehicle. Lysates were subjected to kinase activity profiling with Tyrosine Kinase PamChip® arrays containing 144 kinase peptide substrates. In our experimental model, we were not able to detect a statistically significant large-scale change in ex vivo array peptide phosphorylation by lysates from monocytes treated for 15 minutes. Targets of the IL-10 anti-inflammatory response were not identified. A profound inhibition of array peptide phosphorylation by monocytes treated for 60 minutes was identified, suggesting low activity of a large number of kinases associated with different signaling pathways and immune cell functions, including STAT3 activity, Nf-κB and VEGF signaling, and PTEN signaling activity. The peptide representing ZBTB16, which was reduced in phosphorylation by lysates from all three experimental conditions, was in Ingenuity Pathway Analysis identified to be linked to reduced cytokine release and mRNA levels of tumor necrosis factor (TNF), IL-6, and CXCL10. Further studies should investigate changes in tyrosine kinase-mediated signal transduction in human immune cells, in order to evaluate the potential clinical application of kinome profiling in the study of systemic inflammatory responses to pathogens.http://europepmc.org/articles/PMC5774972?pdf=render
collection DOAJ
language English
format Article
sources DOAJ
author Unni Gopinathan
Kathrine Røe Redalen
Anne-Marie Trøseid
Peter Kierulf
Petter Brandtzaeg
Anne Hansen Ree
Jens Petter Berg
Reidun Øvstebø
spellingShingle Unni Gopinathan
Kathrine Røe Redalen
Anne-Marie Trøseid
Peter Kierulf
Petter Brandtzaeg
Anne Hansen Ree
Jens Petter Berg
Reidun Øvstebø
Large-scale reduction of tyrosine kinase activities in human monocytes stimulated in vitro with N. meningitidis.
PLoS ONE
author_facet Unni Gopinathan
Kathrine Røe Redalen
Anne-Marie Trøseid
Peter Kierulf
Petter Brandtzaeg
Anne Hansen Ree
Jens Petter Berg
Reidun Øvstebø
author_sort Unni Gopinathan
title Large-scale reduction of tyrosine kinase activities in human monocytes stimulated in vitro with N. meningitidis.
title_short Large-scale reduction of tyrosine kinase activities in human monocytes stimulated in vitro with N. meningitidis.
title_full Large-scale reduction of tyrosine kinase activities in human monocytes stimulated in vitro with N. meningitidis.
title_fullStr Large-scale reduction of tyrosine kinase activities in human monocytes stimulated in vitro with N. meningitidis.
title_full_unstemmed Large-scale reduction of tyrosine kinase activities in human monocytes stimulated in vitro with N. meningitidis.
title_sort large-scale reduction of tyrosine kinase activities in human monocytes stimulated in vitro with n. meningitidis.
publisher Public Library of Science (PLoS)
series PLoS ONE
issn 1932-6203
publishDate 2018-01-01
description N. meningitidis induces extensive gene expression changes in human monocytes, suggesting that complex networks of signaling pathways are activated during meningococcal sepsis. These effects are modulated by the anti-inflammatory cytokine interleukin-10 (IL-10). To further study changes in signal transduction suggested by mRNA data, we used kinase substrate arrays to identify composite kinase activities induced by lysates from a primary human monocyte model system. Cell lysates were prepared from monocytes treated with the following experimental conditions: 106 N. meningitidis/mL, 25 ng/mL IL-10, 106 N. meningitidis/mL in combination with 25 ng/mL IL-10, and vehicle. Lysates were subjected to kinase activity profiling with Tyrosine Kinase PamChip® arrays containing 144 kinase peptide substrates. In our experimental model, we were not able to detect a statistically significant large-scale change in ex vivo array peptide phosphorylation by lysates from monocytes treated for 15 minutes. Targets of the IL-10 anti-inflammatory response were not identified. A profound inhibition of array peptide phosphorylation by monocytes treated for 60 minutes was identified, suggesting low activity of a large number of kinases associated with different signaling pathways and immune cell functions, including STAT3 activity, Nf-κB and VEGF signaling, and PTEN signaling activity. The peptide representing ZBTB16, which was reduced in phosphorylation by lysates from all three experimental conditions, was in Ingenuity Pathway Analysis identified to be linked to reduced cytokine release and mRNA levels of tumor necrosis factor (TNF), IL-6, and CXCL10. Further studies should investigate changes in tyrosine kinase-mediated signal transduction in human immune cells, in order to evaluate the potential clinical application of kinome profiling in the study of systemic inflammatory responses to pathogens.
url http://europepmc.org/articles/PMC5774972?pdf=render
work_keys_str_mv AT unnigopinathan largescalereductionoftyrosinekinaseactivitiesinhumanmonocytesstimulatedinvitrowithnmeningitidis
AT kathrinerøeredalen largescalereductionoftyrosinekinaseactivitiesinhumanmonocytesstimulatedinvitrowithnmeningitidis
AT annemarietrøseid largescalereductionoftyrosinekinaseactivitiesinhumanmonocytesstimulatedinvitrowithnmeningitidis
AT peterkierulf largescalereductionoftyrosinekinaseactivitiesinhumanmonocytesstimulatedinvitrowithnmeningitidis
AT petterbrandtzaeg largescalereductionoftyrosinekinaseactivitiesinhumanmonocytesstimulatedinvitrowithnmeningitidis
AT annehansenree largescalereductionoftyrosinekinaseactivitiesinhumanmonocytesstimulatedinvitrowithnmeningitidis
AT jenspetterberg largescalereductionoftyrosinekinaseactivitiesinhumanmonocytesstimulatedinvitrowithnmeningitidis
AT reidunøvstebø largescalereductionoftyrosinekinaseactivitiesinhumanmonocytesstimulatedinvitrowithnmeningitidis
_version_ 1725127562585178112

Similar Items