Your search keyword '"Joris J T H Roelofs"' showing total 278 results

251. Reply from the authors

Author

Huub C. Gelderblom, Marcel G. W. Dijkgraaf, R. Bart Takkenberg, Marjan J. Tempelmans, Joep de Bruijne, Kathelijne Dik, Joost C. M. Meijers, Henk W. Reesink, Joris J. T. H. Roelofs, Peter L.M. Jansen, and Marcel Levi

Subjects

Infectious Diseases, Letter to the editor, Hepatology, business.industry, Medicine, business, Classics

Published

2012

252. Sa1676 Estrogens Promote Development of Colitis-Associated Cancer

Author

Izak Biemond, Sanne L. Rosekrans, Jarom Heijmans, Mattheus C. B. Wielenga, Daniel W. Hommes, Antwan G. Ederveen, Joris J. T. H. Roelofs, James C. H. Hardwick, Vanesa Muncan, Gijs R. van den Brink, Eveline S. de Jonge Muller, Patrick G. Groothuis, and Jooske F. van Lidth de Jeude

Subjects

Hepatology, business.industry, Gastroenterology, Cancer research, Medicine, Colitis associated cancer, business

Published

2013

253. Front & Back Matter

Author

Yuemei Dong, Sandra Jansen, Thomas Pufe, Jose Luis Ramirez, Peter Aaby, Simone C. Tauber, Cornelis van 't Veer, Frank Preijers, Gee W. Lau, Jude M. Taylor, Johanneke Kleinnijenhuis, Jessica Quintin, Tracy Maddocks, Leo A. B. Joosten, Pavel Hyršl, Emma J. Grant, Zhiyong Ma, Pavel Dobeš, Magdiel Pérez-Cruz, Lucie Kucerova, Rommel Max Tan, Mihai G. Netea, Mengji Lu, Jaring S. van der Zee, Cristina Costa, Zhi Wang, Yonghua Hao, Alvaro Molina-Cruz, Janneth Rodrigues, Zhizhou Kuang, Joke van Loenhout, Florry E. van den Boogaard, Jean Gosselin, Mercedes Monteleone, Amanda Skora, Jason D. McArthur, Marie Ranson, Victor Nizet, Katherine Kedzierska, Jos W. M. van der Meer, George Dimopoulos, Druckerei Stückle, James A. Tsatsaronis, Diane Ly, Alexandre Brunet, Rongjuan Pei, Badrul Arefin, Thekla Kemper, Reinout van Crevel, Carolina Barillas-Mury, Dimitri A. Diavatopoulos, Ulrich Theopold, Luiz Carlos Alves, Fábio André Brayner, Satz Mengensatzproduktion, Alex F. de Vos, Stan de Kleijn, Lea-Jessica Albrecht, Manon Le Bel, Mark J. Walker, Aldert Zomer, Michal Zurovec, Jonas Höss, Arie J. Hoogendijk, Patrick C. Reading, Xiaoyong Zhang, Cortny A. Donald, Nicholas P. West, Robert Markus, Xinwen Chen, Bo Qin, Regina de Beer, Peter W. M. Hermans, Eugenia Kress, Lars-Ove Brandenburg, Hynek Strnad, Martina L. Sanderson-Smith, Lindsey S. Garver, Joerg Schlaak, Marloes Vissers, Tom van der Poll, Christine Stabell Benn, Martin Trippler, Kirsty R. Short, Gerben Ferwerda, Oliver Soehnlein, Wandi Zhu, Joris J. T. H. Roelofs, Ramnik J. Xavier, Cor Jacobs, Rafael Mañez, Julika Merres, J. Daan de Boer, Jack Yang, and April M. Clayton

Subjects

Optics, business.industry, Immunology and Allergy, business, Geology, Front (military)

Published

2013

254. Comment on 'Tissue Factor-Dependent Chemokine Production Aggravates Experimental Colitis'

Author

Marleen I. Verstege, Anje A. te Velde, Angelique P. Groot, Joris J. T. H. Roelofs, Henri H. Versteeg, C. Arnold Spek, Karla C. S. Queiroz, JanWillem Duitman, Hella L. Aberson, Cornelis van 't Veer, Yascha W. van den Berg, Faculteit der Geneeskunde, Other departments, ACS - Amsterdam Cardiovascular Sciences, AII - Amsterdam institute for Infection and Immunity, Center of Experimental and Molecular Medicine, CCA -Cancer Center Amsterdam, Pathology, AGEM - Amsterdam Gastroenterology Endocrinology Metabolism, and Tytgat Institute for Liver and Intestinal Research

Subjects

Male, Granulocyte migration, Chemokine, Colon, medicine.medical_treatment, Enzyme-Linked Immunosorbent Assay, Inflammation, Granulocyte, Severity of Illness Index, Inflammatory bowel disease, Thromboplastin, Tissue Culture Techniques, Mice, Tissue factor, Text mining, Cell Movement, Genetics, Animals, Edema, Humans, Medicine, Colitis, Letters to the Editor, Molecular Biology, Genetics (clinical), Mice, Knockout, biology, business.industry, Dextran Sulfate, Experimental colitis, Articles, medicine.disease, Immunohistochemistry, Molecular medicine, Mice, Inbred C57BL, medicine.anatomical_structure, Cytokine, Immunology, Cancer research, biology.protein, Molecular Medicine, Female, Chemokines, Inflammation Mediators, medicine.symptom, business, Granulocytes

Abstract

Tissue factor (TF) is traditionally known as the initiator of blood coagulation, but TF also plays an important role in inflammatory processes. Considering the pivotal role of coagulation in inflammatory bowel disease, we assessed whether genetic ablation of TF limits experimental colitis. To this end, wild-type and TF-deficient (TFlow) mice were treated with 1.5% dextran sulfate sodium (DSS) for 7 d, and effects on disease severity, cytokine production and leukocyte recruitment were examined. Clinical and histological parameters showed that the severity of colitis was reduced in both heterozygous and homozygous TFlow mice compared with controls. Most notably, edema, granulocyte numbers at the site of inflammation and cytokine levels were reduced in TFlow mice. Although anticoagulant treatment with dalteparin of wild-type mice reduced local fibrin production and cytokine levels to a similar extent as in TFlow mice, it did not affect clinical and histological parameters of experimental colitis. Mechanistic studies revealed that IF expression did not influence the intrinsic capacity of granulocytes to migrate. Instead, TF enhanced granulocyte migration into the colon by inducing high levels of the granulocyte chemoattractant keratinocyte-derived chemokine (KC). Taken together, our data indicate that TF plays a detrimental role in experimental colitis by signal transduction-dependent KC production in colon epithelial cells, thereby provoking granulocyte influx with subsequent inflammation and organ damage. (C) 2011 The Feinstein Institute for Medical Research, www.feinsteininstitute.org Online address: http://www.molmed.org doi: 10.2119/molmed.2011.00138

Published

2011

255. PREDICTING LATE INTERSTITIAL FIBROSIS/TUBULAR ATROPHY IN KIDNEY ALLOGRAFTS: A ROLE FOR CD44 EXPRESSION ON RENAL TUBULI

Author

Jesper Kers, I. J. M. ten Berge, Yi-Chun Xu-Dubois, S. Florquin, Joris J. T. H. Roelofs, F. J. Bemelman, Mirza M. Idu, and Eric Rondeau

Subjects

Transplantation, Pathology, medicine.medical_specialty, Kidney, medicine.anatomical_structure, biology, business.industry, Tubular atrophy, CD44, biology.protein, Medicine, Interstitial fibrosis, business

Published

2010

256. Mechanical ventilation aggravates transfusion-related acute lung injury induced by MHC class I antibodies

Author

L Boon, Esther K. Wolthuis, Alexander P.J. Vlaar, MJ Schultz, René Lutter, Joris J. T. H. Roelofs, Jorrit J. Hofstra, and Nicole P. Juffermans

Subjects

Mechanical ventilation, Pathology, medicine.medical_specialty, education.field_of_study, biology, business.industry, Critically ill, medicine.medical_treatment, Population, Lung injury, Critical Care and Intensive Care Medicine, medicine.disease, Immunology, MHC class I, Poster Presentation, medicine, biology.protein, Antibody, Risk factor, education, business, Transfusion-related acute lung injury

Abstract

Transfusion-related acute lung injury (TRALI) occurs more often in critically ill patients than in a general hospital population, possibly due to the presence of underlying inflammatory conditions that may prime pulmonary neutrophils. Mechanical ventilation (MV) may be a risk factor for developing TRALI. We determined the influence of MV on the development of TRALI, combining a murine MV model causing ventilator-induced lung injury with a model of antibody-induced TRALI [1,2].

Published

2010

257. Activated protein C ameliorates coagulopathy but does not influence outcome in lethal H1N1 influenza: a controlled laboratory study

Author

Bruce Gerlitz, Cornelis van 't Veer, Joris J. T. H. Roelofs, Marcel Levi, Tom van der Poll, Koenraad F. van der Sluijs, Marcel Schouten, Brian W. Grinnell, Faculteit der Geneeskunde, Pulmonology, Experimental Immunology, Intensive Care Medicine, Amsterdam Cardiovascular Sciences, Amsterdam institute for Infection and Immunity, Pathology, Vascular Medicine, Center of Experimental and Molecular Medicine, and Infectious diseases

Subjects

Lung, Fibrin degradation product, business.industry, medicine.medical_treatment, Lethal dose, Inflammation, Lung injury, Critical Care and Intensive Care Medicine, respiratory tract diseases, medicine.anatomical_structure, Fibrinolysis, Immunology, medicine, medicine.symptom, business, Plasminogen activator, Protein C, medicine.drug

Abstract

Introduction: Influenza accounts for 5 to 10% of community-acquired pneumonias and is a major cause of mortality. Sterile and bacterial lung injuries are associated with procoagulant and inflammatory derangements in the lungs. Activated protein C (APC) is an anticoagulant with anti-inflammatory properties that exert beneficial effects in models of lung injury. We determined the impact of lethal influenza A (H1N1) infection on systemic and pulmonary coagulation and inflammation, and the effect of recombinant mouse (rm-) APC hereon. Methods: Male C57BL/6 mice were intranasally infected with a lethal dose of a mouse adapted influenza A (H1N1) strain. Treatment with rm-APC (125 mu g intraperitoneally every eight hours for a maximum of three days) or vehicle was initiated 24 hours after infection. Mice were euthanized 48 or 96 hours after infection, or observed for up to nine days. Results: Lethal H1N1 influenza resulted in systemic and pulmonary activation of coagulation, as reflected by elevated plasma and lung levels of thrombin-antithrombin complexes and fibrin degradation products. These procoagulant changes were accompanied by inhibition of the fibrinolytic response due to enhanced release of plasminogen activator inhibitor type-1. Rm-APC strongly inhibited coagulation activation in both plasma and lungs, and partially reversed the inhibition of fibrinolysis. Rm-APC temporarily reduced pulmonary viral loads, but did not impact on lung inflammation or survival. Conclusions: Lethal influenza induces procoagulant and antifibrinolytic changes in the lung which can be partially prevented by rm-APC treatment

Published

2010

258. Urokinase receptor is necessary for bacterial defense against Gram-negative sepsis (melioidosis) by facilitating phagoctytosis

Author

Nicholas P. J. Day, Arjen M. Dondorp, Sharon J. Peacock, Gjw van der Windt, Joris J. T. H. Roelofs, Jwr Hovius, M.M. Levi, T. van der Poll, Jcm Meijers, and W. Joost Wiersinga

Subjects

Melioidosis, biology, business.industry, Burkholderia pseudomallei, medicine.medical_treatment, Gram negative sepsis, Inflammation, bacterial infections and mycoses, Critical Care and Intensive Care Medicine, medicine.disease, biology.organism_classification, Sepsis, Urokinase receptor, Fibrinolysis, Immunology, Poster Presentation, Medicine, medicine.symptom, business, neoplasms, Bacteria

Abstract

Urokinase receptor (uPAR, CD87), a glycosylphosphatidylinositol-anchored protein, is considered to play an important role in inflammation and fibrinolysis. The Gram-negative bacterium Burkholderia pseudomallei is able to survive and replicate within leukocytes and causes melioidosis, an important cause of pneumonia-derived community-acquired sepsis in Southeast Asia. We here investigated the expression and function of uPAR both in patients with septic melioidosis and in a murine model of experimental melioidosis.

Published

2009

259. Recombinant human tissue factor pathway inhibitor exerts anticoagulant, anti-inflammatory and antibacterial effects in murine pneumococcal pneumonia

Author

F. E. van den Boogaard, MJ Schultz, Xanthe Brands, Marcel Levi, T. van der Poll, C. van 't Veer, and Joris J. T. H. Roelofs

Subjects

business.industry, medicine.medical_treatment, Critical Care and Intensive Care Medicine, medicine.disease, medicine.disease_cause, respiratory tract diseases, Sepsis, Tissue factor, Pneumonia, Tissue factor pathway inhibitor, Coagulation, Pneumococcal pneumonia, Fibrinolysis, Immunology, Streptococcus pneumoniae, Poster Presentation, medicine, business

Abstract

Streptococcus pneumoniae is the most common causative pathogen in community-acquired pneumonia and a major cause of sepsis. Pneumonia elicits a procoagulant state in the lung resulting from activation of coagulation, downregulation of anticoagulant pathways and concurrent inhibition of fibrinolysis. Tissue factor is the main initiator of coagulation. Recombinant human tissue factor pathway inhibitor (rh-TFPI) attenuates sepsis-induced coagulation and has been evaluated in clinical trials involving patients with sepsis and community-acquired pneumonia.

Published

2009

260. Inflammation patterns induced by different Burkholderia species in mice

Author

Tom van der Poll, Donald E. Woods, Catharina W. Wieland, Alex F. de Vos, Regina de Beer, W. Joost Wiersinga, Joris J. T. H. Roelofs, Infectious diseases, Center of Experimental and Molecular Medicine, Amsterdam institute for Infection and Immunity, Other departments, Amsterdam Cardiovascular Sciences, and Pathology

Subjects

Chemokine, Melioidosis, Burkholderia, Immunology, Colony Count, Microbial, Virulence, Spleen, Inflammation, Microbiology, Mice, In vivo, Virology, medicine, Animals, Lung, Peroxidase, biology, Burkholderia pseudomallei, bacterial infections and mycoses, medicine.disease, biology.organism_classification, Survival Analysis, Mice, Inbred C57BL, Mutagenesis, Insertional, Blood, medicine.anatomical_structure, DNA Transposable Elements, biology.protein, Cytokines, bacteria, medicine.symptom, Granulocytes

Abstract

Summary Burkholderia pseudomallei, which causes melioidosis, a severe, mainly pulmonary disease endemic in South-East Asia, is considered to be the most pathogenic of the Burkholderia genus. B. thailandensis, however, is considered avirulent. We determined differences in patterns of inflammation of B. pseudomallei 1026b (clinical virulent isolate), B. pseudomallei AJ1D8 (an in vitro invasion-deficient mutant generated from strain 1026b by Tn5-OT182 mutagenesis) and B. thailandensis by intranasally inoculating C57BL/6 mice with each strain. Mice infected with B. thailandensis showed a markedly decreased bacterial outgrowth from lungs, spleen and blood 24 h after inoculation, compared with infection with B. pseudomallei and the invasion mutant AJ1D8. Forty-eight hours after inoculation, B. thailandensis was no longer detectable. This was consistent with elevated pulmonary cytokine and chemokine concentrations after infection with B. pseudomallei 1026b and AJ1D8, and the absence of these mediators 48 h, but not 24 h, after inoculation with B. thailandensis. Histological examination, however, did show marked pulmonary inflammation in the mice infected with B. thailandensis, corresponding with substantial granulocyte influx and raised myeloperoxidase levels. Survival experiments showed that infection with 1 × 103 cfu B. thailandensis was not lethal, whereas inoculation with 1 × 106 cfu B. thailandensis was equally lethal as 1 × 103 cfu B. pseudomallei 1026b or AJ1D8. These data show that B. pseudomallei AJ1D8 is just as lethal as wild-type B. pseudomallei in an in vivo mouse model, and B. thailandensis is perhaps more virulent than is often recognized.

Published

2007

261. Pre-transplant plasma and cellular levels of CD44 correlate with acute renal allograft rejection.

Author

Kasper M. A. Rouschop and Joris J. T. H. Roelofs

Abstract

Background. Since CD44 is involved in activation, proliferation, rolling and extravasation of lymphocytes, we hypothesized that it could be involved in the pathophysiology of acute renal allograft rejection.Methods. Plasma and peripheral blood mononuclear cells (PBMCs) were collected from patients 24 h prior to transplantation and analysed retrospectively. Soluble CD44, interleukin-2 receptor (IL-2R), intracellular adhesion molecule-1 (ICAM-1) and C-reactive protein (CRP) in plasma were determined by enzyme-linked immunosorbent assay (ELISA). Cellular CD44 expression on peripheral lymphocytes was determined by flow cytometric analysis.Results. Patients who later developed renal allograft rejection had statistically significantly increased soluble CD44 levels, but not soluble ICAM-1, IL-2R or CRP in plasma prior to transplantation. In addition, cellular CD44 on T-lymphocytes was decreased 24 h prior to transplantation in patients that would reject their allograft, compared with patients without rejection. Additionally, plasma CD44 and cellular CD44 revealed an inversely proportional correlation. Lipopolysaccharide (LPS)-induced immune activation did not influence plasma or cellular CD44 levels in healthy volunteers, suggesting that more specific factors influence the shedding of CD44 on T lymphocytes, leading to increased risk of renal allograft rejection.Conclusion. Although the exact mechanism remains to be elucidated and further research is required, soluble CD44 levels and cellular surface CD44 on T lymphocytes prior to transplantation might be useful as predictive markers for the occurrence of acute renal rejection. [ABSTRACT FROM AUTHOR]

Published

2005

262. Nebulized C1-Esterase Inhibitor does not Reduce Pulmonary Complement Activation in Rats with Severe Streptococcus Pneumoniae Pneumonia

Author

Gerie J. Glas, Wim K. Lagrand, Marcus J. Schultz, Nicole P. Juffermans, Gerard van Mierlo, Diana Wouters, Charlotte J. P. Beurskens, Sacha Zeerleder, Joris J. T. H. Roelofs, Janneke Horn, Friso M. de Beer, Amsterdam Neuroscience - Neuroinfection & -inflammation, Anesthesiology, Other departments, Landsteiner Laboratory, Clinical Haematology, Pathology, and Intensive Care Medicine

Subjects

Male, 0301 basic medicine, 030204 cardiovascular system & hematology, medicine.disease_cause, Severity of Illness Index, Biochemistry, Rats, Sprague-Dawley, Pathogenesis, 0302 clinical medicine, Pulmonary complement activation, Complement Activation, Lung, Complement C4, General Medicine, respiratory system, Lung injury, Streptococcus pneumoniae, medicine.anatomical_structure, Tumor necrosis factor alpha, medicine.symptom, Bronchoalveolar Lavage Fluid, Complement C1 Inhibitor Protein, Lung inflammation, Complement, Biophysics, Enzyme-Linked Immunosorbent Assay, Inflammation, 03 medical and health sciences, Complement inhibition, medicine, Animals, C1-esterase inhibitor, Original Paper, Interleukin-6, Tumor Necrosis Factor-alpha, business.industry, Pneumonia, Cell Biology, medicine.disease, Rats, Complement system, respiratory tract diseases, Disease Models, Animal, 030104 developmental biology, Case-Control Studies, Immunology, Pulmonary inflammation, business

Abstract

Complement activation plays an important role in the pathogenesis of pneumonia. We hypothesized that inhibition of the complement system in the lungs by repeated treatment with nebulized plasma-derived human C1-esterase inhibitor reduces pulmonary complement activation and subsequently attenuates lung injury and lung inflammation. This was investigated in a rat model of severeStreptococcus pneumoniaepneumonia. Rats were intra–tracheally challenged withS. pneumoniaeto induce pneumonia. Nebulized C1-esterase inhibitor or saline (control animals) was repeatedly administered to rats, 30 min before induction of pneumonia and every 6 h thereafter. Rats were sacrificed 20 or 40 h after inoculation with bacteria. Brochoalveolar lavage fluid and lung tissue were obtained for measuring levels of complement activation (C4b/c), lung injury and inflammation. Induction of pneumonia was associated with pulmonary complement activation (C4b/c at 20 h 1.24 % [0.56–2.59] and at 40 h 2.08 % [0.98–5.12], compared to 0.50 % [0.07–0.59] and 0.03 % [0.03–0.03] in the healthy control animals). The functional fraction of C1-INH was detectable in BALF, but no effect was found on pulmonary complement activation (C4b/c at 20 h 0.73 % [0.16–1.93] and at 40 h 2.38 % [0.54–4.19]). Twenty hours after inoculation, nebulized C1-esterase inhibitor treatment reduced total histology score, but this effect was no longer seen at 40 h. Nebulized C1-esterase inhibitor did not affect other markers of lung injury or lung inflammation. In this negative experimental animal study, severeS. pneumoniaepneumonia in rats is associated with pulmonary complement activation. Repeated treatment with nebulized C1-esterase inhibitor, although successfully delivered to the lungs, does not affect pulmonary complement activation, lung inflammation or lung injury.

263. Neutrophil extracellular traps in the host defense against sepsis induced by Burkholderia pseudomallei (melioidosis)

Author

Sharon J. Peacock, Hanna K. de Jong, Gavin C. K. W. Koh, Nicholas P. J. Day, Ingrid Bulder, Anne Jan van der Meer, Joris J. T. H. Roelofs, Sacha Zeerleder, Femke Stephan, Ahmed Achouiti, W. Joost Wiersinga, Infectious diseases, Amsterdam institute for Infection and Immunity, Graduate School, Other departments, Amsterdam Cardiovascular Sciences, Pathology, and Clinical Haematology

Subjects

Burkholderia pseudomallei, Melioidosis, Survival, Neutrophils, Inflammation, Critical Care and Intensive Care Medicine, Systemic inflammation, Microbiology, Sepsis, DNase, medicine, Innate immunity, biology, business.industry, Research, Diabetes, Elastase, Neutrophil extracellular traps, medicine.disease, biology.organism_classification, bacterial infections and mycoses, 3. Good health, Neutrophil elastase, Immunology, Neutrophil extracellular traps (NETs), biology.protein, medicine.symptom, business

Abstract

Background Neutrophil extracellular traps (NETs) are a central player in the host response to bacteria: neutrophils release extracellular DNA (nucleosomes) and neutrophil elastase to entrap and kill bacteria. We studied the role of NETs in Burkholderia pseudomallei infection (melioidosis), an important cause of Gram-negative sepsis in Southeast Asia. Methods In a prospective observational study, circulating nucleosomes and neutrophil elastase were assayed in 44 patients with Gram-negative sepsis caused by B. pseudomallei (melioidosis) and 82 controls. Functional assays included human neutrophil stimulation and killing assays and a murine model of B. pseudomallei infection in which NET function was compromised using DNase. Specified pathogen-free 8- to 12-week-old C57BL/6 mice were sacrificed post-infection to assess bacterial loads, inflammation, and pathology. Results Nucleosome and neutrophil elastase levels were markedly elevated in patients compared to controls. NETs killed B. pseudomallei effectively, and neutrophils stimulated with B. pseudomallei showed increased elastase and DNA release in a time- and dose-dependent matter. In mice, NET disruption with intravenous DNase administration resulted in decreased nucleosome levels. Although DNase treatment of mice resulted in diminished liver inflammation, no differences were observed in bacterial dissemination or systemic inflammation. Conclusion B. pseudomallei is a potent inducer of NETosis which was reflected by greatly increased levels of NET-related components in melioidosis patients. Although NETs exhibited antibacterial activity against B. pseudomallei, NET formation did not protect against bacterial dissemination and inflammation during B. pseudomallei-induced sepsis. Electronic supplementary material The online version of this article (doi:10.1186/s40635-014-0021-2) contains supplementary material, which is available to authorized users.

264. Topical adjunctive treatment with flagellin augments pulmonary neutrophil responses and reduces bacterial dissemination in multidrug-resistant K. pneumoniae infection

Author

Christine C. A. van Linge, Robert F.J. Kullberg, Osoul Chouchane, Joris J. T. H. Roelofs, Wil H. F. Goessens, Cornelis van ‘t Veer, Jean-Claude Sirard, Alex F. de Vos, and Tom van der Poll

Subjects

pneumonia, Klebsiella pneumoniae, antimicrobial resistance, flagellin, respiratory infection, Immunologic diseases. Allergy, RC581-607

Abstract

ObjectiveAntimicrobial resistance is an emerging problem and multi-drug resistant (MDR) Klebsiella pneumoniae (K. pneumoniae) represents an enormous risk of failing therapy in hospital-acquired pneumonia. The current study aimed to determine the immunomodulatory effect of topical flagellin in addition to antibiotic treatment during respiratory infection evoked by hypervirulent antibiotic-susceptible and antibiotic-resistant K. pneumoniae in mice.MethodsC57BL6 mice were inoculated intranasally with hypervirulent K. pneumoniae (K2:O1) which was either antibiotic-susceptible or multi-drug resistant. Six hours after infection, mice were treated with antibiotics intraperitoneally and flagellin or vehicle intranasally. Mice were sacrificed 24 hours after infection. Samples were analyzed for bacterial loads and for inflammatory and coagulation markers.ResultsFlagellin therapy induced neutrophil influx in the lung during antibiotic-treated pneumonia evoked by either antibiotic-susceptible or -resistant K. pneumoniae. The pulmonary neutrophil response was matched by elevated levels of neutrophil-attracting chemokines, neutrophil degranulation products, and local coagulation activation. The combined therapy of effective antibiotics and flagellin did not impact K. pneumoniae outgrowth in the lung, but decreased bacterial counts in distant organs. Neutrophil depletion abrogated the flagellin-mediated effect on bacterial dissemination and local coagulation responses.ConclusionTopical flagellin administration as an adjunctive to antibiotic treatment augments neutrophil responses during pneumonia evoked by MDR-K. pneumoniae, thereby reducing bacterial dissemination to distant organs.

Published

2024

265. Effect of antibody-mediated connective tissue growth factor neutralization on lung edema in ventilator-induced lung injury in rats

Author

Charissa E. van den Brom, Caitlin Bozic, Chantal A. Polet, Annabel Bongers, Anita M. Tuip-de Boer, Roselique Ibelings, Joris J. T. H. Roelofs, and Nicole P. Juffermans

Subjects

ARDS, CTGF, Edema, Lung, Ventilator-induced lung injury, Therapeutics. Pharmacology, RM1-950, Biochemistry, QD415-436

Abstract

Abstract Background Acute respiratory distress syndrome (ARDS) is characterized by alveolar edema that can progress to septal fibrosis. Mechanical ventilation can augment lung injury, termed ventilator-induced lung injury (VILI). Connective tissue growth factor (CTGF), a mediator of fibrosis, is increased in ARDS patients. Blocking CTGF inhibits fibrosis and possibly vascular leakage. This study investigated whether neutralizing CTGF reduces pulmonary edema in VILI. Methods Following LPS administration, rats were mechanically ventilated for 6 h with low (6 mL/kg; low VT) or moderate (10 mL/kg; mod VT) tidal volume and treated with a neutralizing CTGF antibody (FG-3154) or placebo lgG (vehicle). Control rats without LPS were ventilated for 6 h with low VT. Lung wet-to-dry weight ratio, FITC-labeled dextran permeability, histopathology, and soluble RAGE were determined. Results VILI was characterized by reduced PaO2/FiO2 ratio (low VT: 540 [381–661] vs. control: 693 [620–754], p 0.99), extravasated dextrans (mod VT + FG-3154: 0.06 [0.04–0.09] vs. mod VT + vehicle: 0.04 [0.03–0.09] µg/mg tissue, p > 0.99), sRAGE (mod VT + FG-3154: 1865 [1628–2252] vs. mod VT + vehicle: 1885 [1695–2159] pg/mL, p > 0.99) or histopathology. Conclusions ‘Double hit’ VILI was characterized by inflammation, impaired oxygenation, pulmonary edema and histopathological lung injury. Blocking CTGF does not improve oxygenation nor reduce pulmonary edema in rats with VILI. Graphical Abstract

Published

2024

266. Obesity aggravates acute kidney injury resulting from ischemia and reperfusion in mice

Author

Igor Oliveira da Silva, Nicole K. de Menezes, Heloisa D. Jacobina, Antonio Carlos Parra, Felipe Lima Souza, Leticia Cardoso Castro, Joris J. T. H. Roelofs, Alessandra Tammaro, Samirah Abreu Gomes, Talita Rojas Sanches, and Lucia Andrade

Subjects

Medicine, Science

Abstract

Abstract In critically ill patients, overweight and obesity are associated with acute respiratory distress syndrome and acute kidney injury (AKI). However, the effect of obesity on ischemia–reperfusion injury (IRI)-induced AKI is unknown. We hypothesized that obesity would aggravate renal IRI in mice. We fed mice a standard or high-fat diet for eight weeks. The mice were divided into four groups and submitted to sham surgery or IRI: obese, normal, normal + IRI, obese, and obese + IRI. All studies were performed 48 h after the procedures. Serum glucose, cholesterol, and creatinine clearance did not differ among the groups. Survival and urinary osmolality were lower in the obese + IRI group than in the normal + IRI group, whereas urinary neutrophil gelatinase-associated lipocalin levels, tubular injury scores, and caspase 3 expression were higher. Proliferating cell nuclear antigen expression was highest in the obese + IRI group, as were the levels of oxidative stress (urinary levels of thiobarbituric acid-reactive substances and renal heme oxygenase-1 protein expression), whereas renal Klotho protein expression was lowest in that group. Expression of glutathione peroxidase 4 and peroxiredoxin 6, proteins that induce lipid peroxidation, a hallmark of ferroptosis, was lower in the obese + IRI group. Notably, among the mice not induced to AKI, macrophage infiltration was greater in the obese group. In conclusion, greater oxidative stress and ferroptosis might aggravate IRI in obese individuals, and Klotho could be a therapeutic target in those with AKI.

Published

2024

267. Protease-activated receptor-1 impairs host defense in murine pneumococcal pneumonia: a controlled laboratory study

Author

Marcel Schouten, Joris J. T. H. Roelofs, Cornelis van 't Veer, Tom van der Poll, Marcel Levi, Amsterdam Cardiovascular Sciences, Amsterdam institute for Infection and Immunity, Center of Experimental and Molecular Medicine, Pathology, Vascular Medicine, and Infectious diseases

Subjects

Proteases, Lung, business.industry, Spleen, Inflammation, medicine.disease, medicine.disease_cause, Critical Care and Intensive Care Medicine, Pneumonia, medicine.anatomical_structure, Immunology, Streptococcus pneumoniae, Pneumococcal pneumonia, medicine, medicine.symptom, business, Pathogen

Abstract

Streptococcus pneumoniae is the most common causative pathogen in community-acquired pneumonia. Protease-activated receptor-1 (PAR-1) is expressed by multiple cell types present in the lungs and can be activated by various proteases generated during acute inflammation. The cellular effect of PAR-1 activation partially depends on the specific protease involved. We here determined the role of PAR-1 in the host response during murine pneumococcal pneumonia. Wild-type (WT) and PAR-1 knockout (KO) mice were infected intranasally with viable S. pneumoniae and observed in a survival study or euthanized at 6, 24 or 48 hours of infection. PAR-1 KO mice had a better survival early after infection compared to WT mice. Moreover, PAR-1 KO mice had lower bacterial loads in lungs and blood at 24 hours and in spleen and liver at 48 hours after infection. This favorable response was accompanied by lower lung histopathology scores and less neutrophil influx in PAR-1 KO mice. PAR-1 impairs host defense during murine pneumococcal pneumonia.

268. The effects of resuscitation with different plasma products on endothelial permeability and organ injury in a rat pneumosepsis model

Author

Daan P. van den Brink, Derek J. B. Kleinveld, Annabel Bongers, Jaël Vos, Joris J. T. H. Roelofs, Nina C. Weber, Jaap D. van Buul, and Nicole P. Juffermans

Subjects

Albumin, Endothelial dysfunction, Plasma, Resuscitation, Sepsis, Shock, Medical emergencies. Critical care. Intensive care. First aid, RC86-88.9

Abstract

Abstract Background Endothelial injury and permeability are a hallmark of sepsis. Initial resuscitation of septic patients with crystalloids is associated with aggravation of endothelial permeability, which may be related either to low protein content or to volume. We investigated whether initial resuscitation with different types of plasma or albumin decreases endothelial dysfunction and organ injury in a pneumosepsis rat model compared to the same volume of crystalloids. Study design and methods Sprague–Dawley rats were intratracheally inoculated with Streptococcus pneumoniae. Twenty-four hours after inoculation, animals were randomized to 2 control groups and 5 intervention groups (n = 11 per group) to receive resuscitation with a fixed volume (8 mL/kg for 1 h) of either Ringer’s Lactate, 5% human albumin, fresh frozen plasma derived from syngeneic donor rats (rFFP), human-derived plasma (hFFP) or human-derived solvent detergent plasma (SDP). Controls were non-resuscitated (n = 11) and healthy animals. Animals were sacrificed 5 h after start of resuscitation (T = 5). Pulmonary FITC-dextran leakage as a reflection of endothelial permeability was used as the primary outcome. Results Inoculation with S. Pneumoniae resulted in sepsis, increased median lactate levels (1.6–2.8 mM, p

Published

2023

269. Author Correction: Obesity aggravates acute kidney injury resulting from ischemia and reperfusion in mice

Author

Igor Oliveira da Silva, Nicole K. de Menezes, Heloisa D. Jacobina, Antonio Carlos Parra, Felipe Lima Souza, Leticia Cardoso Castro, Joris J. T. H. Roelofs, Alessandra Tammaro, Samirah Abreu Gomes, Talita Rojas Sanches, and Lucia Andrade

Subjects

Medicine, Science

Published

2024

270. Endogenous tissue-type plasminogen activator is protective during ascending urinary tract infection.

Author

Joris J. T. H. Roelofs, Kasper M. A. Rouschop, Gwendoline J. D. Teske, Gerry T. M. Wagenaar, Nike Claessen, Jan J. Weening, Tom van der Poll, and Sandrine Florquin

Subjects

*TISSUE plasminogen activator, *URINARY tract infections, *PYELONEPHRITIS, *LABORATORY mice, *PHAGOCYTOSIS, *ESCHERICHIA coli

Abstract

Background. Acute pyelonephritis is one of the most common bacterial infections. Tissue-type plasminogen activator (tPA) is a potent fibrinolytic agent, but can play a role in inflammatory processes as well. Methods. We induced pyelonephritis in tPA−/− and C57BL/6 wild-type (WT) mice by intravesical inoculation with 1010 CFU uropathogenic Escherichia coli 1677. The mice were killed after 24 and 48 h, after which bacterial outgrowth and cytokine levels in kidney homogenates were determined. Influx of neutrophils was quantified by myeloperoxidase-ELISA. Neutrophil phagocytosis and oxidative burst were measured. Results. The tPA−/− kidneys contained significantly higher numbers of E. coli CFU, accompanied by higher levels of interleukin-1β (IL-1β) and tumour necrosis factor-α (TNF-α). The number of infiltrating neutrophils was similar in tPA−/− and WT mice at both time points, suggesting that tPA−/− neutrophils have a lower ability to eliminate E. coli. Phagocytosis of E. coli organisms was not diminished in tPA−/− neutrophils. Interestingly, tPA−/− neutrophils showed a significantly lower ability to generate an oxidative burst reaction upon stimulation with E. coli than WT neutrophils. Incubation with recombinant tPA reversed this effect completely. Conclusions. These results show that deletion of the tPA-gene in mice leads to lower bactericidal potential of tPA−/− neutrophils, which results in significantly more bacterial outgrowth during experimental pyelonephritis. [ABSTRACT FROM AUTHOR]

Published

2009

271. Myeloid liver kinase B1 contributes to lung inflammation induced by lipoteichoic acid but not by viable Streptococcus pneumoniae

Author

Liza Pereverzeva, Natasja A. Otto, Joris J. T. H. Roelofs, Alex F. de Vos, and Tom van der Poll

Subjects

Liver kinase B1, Streptococcus pneumoniae, Lipoteichoic acid, Pneumonia, Alveolar macrophages, Diseases of the respiratory system, RC705-779

Abstract

Abstract Background Liver kinase B1 (Lkb1, gene name Stk11) functions as a tumor suppressor in cancer. Myeloid cell Lkb1 potentiates lung inflammation induced by the Gram-negative bacterial cell wall component lipopolysaccharide and in host defense during Gram-negative pneumonia. Here, we sought to investigate the role of myeloid Lkb1 in lung inflammation elicited by the Gram-positive bacterial cell wall component lipoteichoic acid (LTA) and during pneumonia caused by the Gram-positive respiratory pathogen Streptococcus pneumoniae (Spneu). Methods Alveolar and bone marrow derived macrophages (AMs, BMDMs) harvested from myeloid-specific Lkb1 deficient (Stk11-ΔM) and littermate control mice were stimulated with LTA or Spneu in vitro. Stk11-ΔM and control mice were challenged via the airways with LTA or infected with Spneu in vivo. Results Lkb1 deficient AMs and BMDMs produced less tumor necrosis factor (TNF)α upon activation by LTA or Spneu. During LTA-induced lung inflammation, Stk11-ΔM mice had reduced numbers of AMs in the lungs, as well as diminished cytokine release and neutrophil recruitment into the airways. During pneumonia induced by either encapsulated or non-encapsulated Spneu, Stk11-ΔM and control mice had comparable bacterial loads and inflammatory responses in the lung, with the exception of lower TNFα levels in Stk11-ΔM mice after infection with the non-encapsulated strain. Conclusion Myeloid Lkb1 contributes to LTA-induced lung inflammation, but is not important for host defense during pneumococcal pneumonia.

Published

2022

272. Prophylactic furosemide to prevent transfusion-associated circulatory overload: a randomized controlled study in rats

Author

Robert B. Klanderman, Joachim J. Bosboom, Denise P. Veelo, Joris J. T. H. Roelofs, Dirk de Korte, Robin van Bruggen, Liffert Vogt, Jaap D. van Buul, Markus W. Hollmann, Margreeth B. Vroom, Nicole P. Juffermans, Bart F. Geerts, and Alexander P. J. Vlaar

Subjects

Medicine, Science

Abstract

Abstract Transfusion-associated circulatory overload (TACO) is the leading cause of transfusion related morbidity and mortality. The only treatment is empirical use of furosemide. Our aim was to investigate if furosemide can prevent TACO. A randomized controlled trial was performed using a previously validated two-hit rat model for TACO. Volume incompliance was induced (first hit) in anemic, anesthetized Lewis rats. Rats were randomized to placebo, low-dose (5 mg kg−1) or high-dose (15 mg kg−1) furosemide-administered prior to transfusion (second-hit) and divided over two doses. Primary outcome was change in left-ventricular end-diastolic pressure (∆LVEDP) pre- compared to post-transfusion. Secondary outcomes included changes in preload, afterload, contractility and systemic vascular resistance, as well as pulmonary outcomes. Furosemide treated animals had a significantly lower ∆LVEDP compared to placebo (p = 0.041), a dose–response effect was observed. ∆LVEDP in placebo was median + 8.7 mmHg (IQR 5.9–11), + 3.9 (2.8–5.6) in the low-dose and 1.9 (− 0.6 to 5.6) in the high-dose group. The effect of furosemide became apparent after 15 min. While urine output was significantly higher in furosemide treated animals (p = 0.03), there were no significant changes in preload, afterload, contractility or systemic vascular resistance. Furosemide rapidly and dose-dependently decreases the rise in hydrostatic pulmonary pressure following transfusion, essential for preventing TACO.

Published

2022

273. Therapeutic application of recombinant human ADAMTS-13 improves shock reversal and coagulation status in a trauma hemorrhage and transfusion rat model

Author

Mathijs R. Wirtz, Daan P. van den Brink, Joris J. T. H. Roelofs, J. Carel Goslings, and Nicole P. Juffermans

Subjects

ADAMTS-13, Hemorrhage, Trauma, Resuscitation, Coagulopathy, Medical emergencies. Critical care. Intensive care. First aid, RC86-88.9

Abstract

Abstract Introduction In hemorrhaging trauma patients, the endothelium is activated, resulting in excessive endothelial synthesis of von Willebrand Factor (vWF), which may enhance micro-thrombi formation, resulting in obstruction of the microcirculation and endothelial injury, aggravating bleeding, as well as contributing to organ failure. Under normal conditions, vWF is cleaved by the metalloprotease ADAMTS-13. After trauma, ADAMTS-13 levels are reduced. Objectives To assess whether recombinant human ADAMTS-13 inhibits endothelial injury and organ failure in a rat trauma-transfusion model. Methods Blood products were prepared from syngeneic rat blood according to blood bank standards. Polytrauma was induced in rats by crush injury to the intestines and liver and by fracture of the femur. The rats were hemorrhaged until a mean arterial pressure (MAP) of 40 mmHg was reached. Rats were randomized to receive transfusion of RBCs, FFPs, and platelets in a 1:1:1 ratio to achieve a MAP of 70 mmHg, with or without the addition of ADAMTS-13 (50 μg/kg). Blood samples were assessed for biochemistry and rotational thromboelastometry (ROTEM). Syndecan-1 and VE-cadherin levels were measured as a reflection of endothelial integrity. The amount of leakage of dextran-FITC from the vascular system to the parenchyma in lungs was quantified. To assess inflammation, IL-6 and IL-8 levels were determined. Organ damage was assessed by histopathology. Results All rats were severely shocked, with no significant differences in shock parameters between groups. Rats treated with ADAMTS-13 showed signs of a more effective shock reversal (higher blood pressure, lower lactate levels) compared to controls. Also, ROTEM parameters of clot formation in rats receiving ADAMTS-13 improved compared to controls, which was mainly platelet-dependent. Syndecan-1 levels relative to baseline trended to be lower in ADAMTS-13 treated rats compared to controls (107 vs 149%, p = 0.08). ADAMTS-13 reduced albuminuria (1.7 vs 4.4 g/L, p < 0.01) and organ-specific inflammation (pulmonary IL-6 243 vs 369 pg/mL, p = 0.08; splenic IL-6 253 vs 307, p = 0.03) compared to controls, but did not improve histopathological scores. Conclusions The use of ADAMTS-13 in a rat trauma-transfusion model improves parameters of shock, platelet-driven coagulation, endothelial damage, and organ inflammation. These results suggest that ADAMTS-13 is important in mediating outcome of trauma. Whether ADAMTS-13 can be used as a therapeutic adjunct to treat bleeding trauma patients remains to be determined.

Published

2020

274. Pulmonary complement depositions in autopsy of critically ill patients have no relation with ARDS

Author

Friso M. de Beer, Mark P. V. Begieneman, Joris J. T. H. Roelofs, Janneke Horn, Hans W. M. Niessen, Marcus J. Schultz, and Wim K. Lagrand

Subjects

Intensive care, ARDS, Autopsy, Complement, Complement activation, Complement deposition, Medical emergencies. Critical care. Intensive care. First aid, RC86-88.9

Abstract

Abstract Background The complement system has frequently been suggested to play a role in the pathophysiology of acute respiratory distress syndrome (ARDS). The current study explored the association between pulmonary depositions of a complement activation product and the clinical diagnosis of ARDS. Methods Lung tissue material from autopsied critically ill patients who died whilst on invasively mechanical ventilation was collected and stained for complement C3d. The diagnosis of ARDS was by the Berlin Definition. Lung injury scores (LIS) and driving pressures were calculated, 48 and 24 h prior to death. A pathologist who remained blinded for the clinical data scored the extent of C3d depositions, using a C3d deposition score (a minimum and maximum score of 0 and 24), and of diffuse alveolar damage (DAD). The primary analysis focused on the association between the C3d deposition score and the clinical diagnosis of ARDS. Secondary analyses focused on associations between the C3d deposition score and the presence of diffuse alveolar damage (DAD) in histopathology, and LIS and driving pressures in the last 2 days before death. Results Of 36 patients of whom autopsy material was available, 12 were diagnosed as having had ARDS. In all patients, C3d depositions were found in various parts of the lungs, and to a different extent. Notably, C3d deposition scores were similar for patients with ARDS and those without ARDS (4.5 [3.3–6.8] vs. 5.0 [4.0–6.0]; not significant). C3d deposition scores were also independent from the presence or absence of DAD, and correlations between C3d scores and LIS and driving pressures prior to death were poor. Conclusion Pulmonary C3d depositions are found in the lungs of all deceased ICU patients, independent of the diagnosis of ARDS. The presence of complement C3d was not associated with the presence of DAD on histopathology and had a poor correlation with ventilation characteristics prior to death.

Published

2019

275. Hypoxia-Inducible Factor-1α in Macrophages, but Not in Neutrophils, Is Important for Host Defense during Klebsiella pneumoniae-Induced Pneumosepsis

Author

Natasja A. Otto, Liza Pereverzeva, Valentine Leopold, Ivan Ramirez-Moral, Joris J. T. H. Roelofs, Jeroen W. J. van Heijst, Alex F. de Vos, and Tom van der Poll

Subjects

Pathology, RB1-214

Abstract

Hypoxia-inducible factor- (HIF-) 1α has been implicated in the ability of cells to adapt to alterations in oxygen levels. Bacterial stimuli can induce HIF1α in immune cells, including those of myeloid origin. We here determined the role of myeloid cell HIF1α in the host response during pneumonia and sepsis caused by the common human pathogen Klebsiella pneumoniae. To this end, we generated mice deficient for HIF1α in myeloid cells (LysM-cre × Hif1αfl/fl) or neutrophils (Mrp8-cre × Hif1αfl/fl) and infected these with Klebsiella pneumoniae via the airways. Myeloid, but not neutrophil, HIF1α-deficient mice had increased bacterial loads in the lungs and distant organs after infection as compared to control mice, pointing at a role for HIF1α in macrophages. Myeloid HIF1α-deficient mice did not show increased bacterial growth after intravenous infection, suggesting that their phenotype during pneumonia was mediated by lung macrophages. Alveolar and lung interstitial macrophages from LysM-cre × Hif1αfl/fl mice produced lower amounts of the immune enhancing cytokine tumor necrosis factor upon stimulation with Klebsiella, while their capacity to phagocytose or to produce reactive oxygen species was unaltered. Alveolar macrophages did not upregulate glycolysis in response to lipopolysaccharide, irrespective of HIF1α presence. These data suggest a role for HIF1α expressed in lung macrophages in protective innate immunity during pneumonia caused by a common bacterial pathogen.

Published

2021

276. Combining streptozotocin and unilateral nephrectomy is an effective method for inducing experimental diabetic nephropathy in the ‘resistant’ C57Bl/6J mouse strain

Author

Melissa Uil, Angelique M. L. Scantlebery, Loes M. Butter, Per W. B. Larsen, Onno J. de Boer, Jaklien C. Leemans, Sandrine Florquin, and Joris J. T. H. Roelofs

Subjects

Medicine, Science

Abstract

Abstract Diabetic nephropathy (DN) is the leading cause of chronic kidney disease. Animal models are essential tools for designing new strategies to prevent DN. C57Bl/6 (B6) mice are widely used for transgenic mouse models, but are relatively resistant to DN. This study aims to identify the most effective method to induce DN in a type 1 (T1D) and a type 2 diabetes (T2D) model in B6 mice. For T1D-induced DN, mice were fed a control diet, and randomised to streptozotocin (STZ) alone, STZ+unilateral nephrectomy (UNx), or vehicle/sham. For T2D-induced DN, mice were fed a western (high fat) diet, and randomised to either STZ alone, STZ+UNx, UNx alone, or vehicle/sham. Mice subjected to a control diet with STZ +UNx developed albuminuria, glomerular lesions, thickening of the glomerular basement membrane, and tubular injury. Mice on control diet and STZ developed only mild renal lesions. Furthermore, kidneys from mice on a western diet were hardly affected by diabetes, UNx or the combination. We conclude that STZ combined with UNx is the most effective model to induce T1D-induced DN in B6 mice. In our hands, combining western diet and STZ treatment with or without UNx did not result in a T2D-induced DN model in B6 mice.

Published

2018

277. Hyperoxia provokes a time- and dose-dependent inflammatory response in mechanically ventilated mice, irrespective of tidal volumes

Author

Hendrik J. F. Helmerhorst, Laura R. A. Schouten, Gerry T. M. Wagenaar, Nicole P. Juffermans, Joris J. T. H. Roelofs, Marcus J. Schultz, Evert de Jonge, and David J. van Westerloo

Subjects

Hyperoxia, Mechanical ventilation, mice, VILI, Inflammation, Oxygen toxicity, Medical emergencies. Critical care. Intensive care. First aid, RC86-88.9

Abstract

Abstract Background Mechanical ventilation and hyperoxia have the potential to independently promote lung injury and inflammation. Our purpose was to study both time- and dose-dependent effects of supplemental oxygen in an experimental model of mechanically ventilated mice. Methods Healthy male C57Bl/6J mice, aged 9–10 weeks, were intraperitoneally anesthetized and randomly assigned to the mechanically ventilated group or the control group. In total, 100 mice were tracheotomized and mechanically ventilated for either 8 or 12 h after allocation to different settings for the applied fractions of inspired oxygen (FiO2, 30, 50, or 90%) and tidal volumes (7.5 or 15 ml/kg). After euthanisation arterial blood, bronchoalveolar lavage fluid (BALf) and tissues were collected for analyses. Results Mechanical ventilation significantly increased the lung injury score (P

Published

2017

278. Relative Tissue Factor Deficiency Attenuates Ventilator-Induced Coagulopathy but Does Not Protect against Ventilator-Induced Lung Injury in Mice

Author

Esther K. Wolthuis, Alexander P. J. Vlaar, Goda Choi, Joris J. T. H. Roelofs, Marcel Levi, Nicole P. Juffermans, and Marcus J. Schultz

Subjects

Medical emergencies. Critical care. Intensive care. First aid, RC86-88.9

Abstract

Preventing tissue-factor-(TF-) mediated systemic coagulopathy improves outcome in models of sepsis. Preventing TF-mediated pulmonary coagulopathy could attenuate ventilator-induced lung injury (VILI). We investigated the effect of relative TF deficiency on pulmonary coagulopathy and inflammation in a murine model of VILI. Heterozygous TF knockout (TF+/−) mice and their wild-type (TF+/+) littermates were sedated (controls) or sedated, tracheotomized, and mechanically ventilated with either low or high tidal volumes for 5 hours. Mechanical ventilation resulted in pulmonary coagulopathy and inflammation, with more injury after mechanical ventilation with higher tidal volumes. Compared with TF+/+ mice, TF+/− mice demonstrated significantly lower pulmonary thrombin-antithrombin complex levels in both ventilation groups. There were, however, no differences in lung wet-to-dry ratio, BALF total protein levels, neutrophil influx, and lung histopathology scores between TF+/− and TF+/+ mice. Notably, pulmonary levels of cytokines were significantly higher in TF+/− as compared to TF+/+ mice. Systemic levels of cytokines were not altered by the relative absence of TF. TF deficiency is associated with decreased pulmonary coagulation independent of the ventilation strategy. However, relative TF deficiency does not reduce VILI and actually results in higher pulmonary levels of inflammatory mediators.

Published

2012