The anti-inflammatory effect of combined complement and CD14 inhibition is preserved during escalating bacterial load

Egge, K.; Barratt‐Due, Andreas; Nymo, Stig Haugset; Lindstad, Julie Katrine; Pharo, Anne; Lau, Corinna; Espevik, Terje; Thorgersen, Ebbe Billmann; Mollnes, Tom Eirik

doi:10.1111/cei.12645

Cited by 8 publications

(7 citation statements)

References 42 publications

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“…Genetic ablation or pharmacological blockade of C5a signalling or C3 activation improves outcomes in animal models of sepsis 81,83,84 . Moreover, in vitro and in vivo studies have provided evidence of synergistic effects of blocking complement and TLRs simultaneously 85,86 , underscoring the crosstalk that occurs between these systems in pathological events. In patients with severe trauma, the presentation of DAMPs after tissue injury can trigger complement activation, which induces SIRS and contributes to complications such as multi-organ dysfunction and/or death 87–89 .…”

Section: Complex Involvement In Clinical Disordersmentioning

confidence: 99%

Complement in disease: a defence system turning offensive

2016

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Although the complement system is primarily perceived as a host defence system, a more versatile, yet potentially more harmful side of this innate immune pathway as an inflammatory mediator also exists. The activities that define the ability of the complement system to control microbial threats and eliminate cellular debris — such as sensing molecular danger patterns, generating immediate effectors, and extensively coordinating with other defence pathways — can quickly turn complement from a defence system to an aggressor that drives immune and inflammatory diseases. These host-offensive actions become more pronounced with age and are exacerbated by a variety of genetic factors and autoimmune responses. Complement can also be activated inappropriately, for example in response to biomaterials or transplants. A wealth of research over the past two decades has led to an increasingly finely tuned understanding of complement activation, identified tipping points between physiological and pathological behaviour, and revealed avenues for therapeutic intervention. This Review summarizes our current view of the key activating, regulatory, and effector mechanisms of the complement system, highlighting important crosstalk connections, and, with an emphasis on kidney disease and transplantation, discusses the involvement of complement in clinical conditions and promising therapeutic approaches.

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Section: Complex Involvement In Clinical Disordersmentioning

confidence: 99%

Complement in disease: a defence system turning offensive

2016

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“…We found that E. coli-induced whole blood-mediated activation of EC was largely CD14-dependent whereas S. aureus-induced activation was mediated by the complement system, mainly through C5a-C5aR1 interaction. We have earlier found that single inhibition is less efficient than combined inhibition, particularly with increased load of inflammatory stimuli (35). In the present study, we used fairly low concentrations of bacteria compared with previous studies in whole blood alone, which might explain the impressive effect of single inhibition.…”

Section: Discussionmentioning

confidence: 86%

Human Endothelial Cell Activation by Escherichia coli and Staphylococcus aureus Is Mediated by TNF and IL-1β Secondarily to Activation of C5 and CD14 in Whole Blood

Nymo

Gustavsen

Nilsson

et al. 2016

The Journal of Immunology

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Endothelial cells (EC) play a central role in inflammation. E-selectin and ICAM-1 expression are essential for leukocyte recruitment and are good markers of EC activation. Most studies of EC activation are done in vitro using isolated mediators. The aim of the present study was to examine the relative importance of pattern recognition systems and downstream mediators in bacteria-induced EC activation in a physiological relevant human model, using EC incubated with whole blood. HUVEC were incubated with human whole blood. Escherichia coli– and Staphylococcus aureus–induced EC activation was measured by E-selectin and ICAM-1 expression using flow cytometry. The mAb 18D11 was used to neutralize CD14, and the lipid A analog eritoran was used to block TLR4/MD2. C5 cleavage was inhibited using eculizumab, and C5aR1 was blocked by an antagonist. Infliximab and canakinumab were used to neutralize TNF and IL-1β. The EC were minimally activated when bacteria were incubated in serum, whereas a substantial EC activation was seen when the bacteria were incubated in whole blood. E. coli–induced activation was largely CD14-dependent, whereas S. aureus mainly caused a C5aR1-mediated response. Combined CD14 and C5 inhibition reduced E-selectin and ICAM-1 expression by 96 and 98% for E. coli and by 70 and 75% for S. aureus. Finally, the EC activation by both bacteria was completely abolished by combined inhibition of TNF and IL-1β. E. coli and S. aureus activated EC in a CD14- and C5-dependent manner with subsequent leukocyte secretion of TNF and IL-1β mediating the effect.

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“…For instance, congruently upregulated genes included the CD14 molecule, the lipopolysaccharide‐binding protein (LBP), and the Toll‐like receptors (TLRs) 2, 4, 6, and 8. CD14 is an accessory receptor for TLRs, and ongoing clinical trials indicate that CD14 inhibition is a promising strategy to treat sepsis (Verbon et al , ; Egge et al , ). Furthermore, LBP is an acute‐phase biomarker for sepsis (Schumann & Zweigner, ), and the TLR family was recently reported to be a promising target for the treatment of sepsis (Savva & Roger, ).…”

Section: Discussionmentioning

confidence: 99%

Defining the optimal animal model for translational research using gene set enrichment analysis

et al. 2016

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The mouse is the main model organism used to study the functions of human genes because most biological processes in the mouse are highly conserved in humans. Recent reports that compared identical transcriptomic datasets of human inflammatory diseases with datasets from mouse models using traditional gene‐to‐gene comparison techniques resulted in contradictory conclusions regarding the relevance of animal models for translational research. To reduce susceptibility to biased interpretation, all genes of interest for the biological question under investigation should be considered. Thus, standardized approaches for systematic data analysis are needed. We analyzed the same datasets using gene set enrichment analysis focusing on pathways assigned to inflammatory processes in either humans or mice. The analyses revealed a moderate overlap between all human and mouse datasets, with average positive and negative predictive values of 48 and 57% significant correlations. Subgroups of the septic mouse models (i.e., Staphylococcus aureus injection) correlated very well with most human studies. These findings support the applicability of targeted strategies to identify the optimal animal model and protocol to improve the success of translational research.

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The anti-inflammatory effect of combined complement and CD14 inhibition is preserved during escalating bacterial load

Cited by 8 publications

References 42 publications

Complement in disease: a defence system turning offensive

Complement in disease: a defence system turning offensive

Human Endothelial Cell Activation by Escherichia coli and Staphylococcus aureus Is Mediated by TNF and IL-1β Secondarily to Activation of C5 and CD14 in Whole Blood

Defining the optimal animal model for translational research using gene set enrichment analysis

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