Your search keyword '"Herwald H"' showing total 12 results

1. Heparin-binding protein as a biomarker of post-injury sepsis in trauma patients.

Author

Halldorsdottir, H. D., Eriksson, J., Persson, B. P., Herwald, H., Lindbom, L., Weitzberg, E., and Oldner, A.

Subjects

HEPARIN, NEUTROPHILS, SEPSIS, MORTALITY, INFLAMMATION, C-reactive protein

Abstract

Background: Heparin-binding protein (HBP) is a neutrophil-derived protein advocated as a biomarker in sepsis. We evaluated plasma HBP as a predictor of post-injury sepsis in trauma patients.Methods: Ninety-seven trauma patients were studied during the first week of intensive care. Injury-related data were collected and clinical parameters registered daily. Plasma HBP was sampled on day 1, 3 and 5 after trauma and evaluated for associations with injury-related parameters and sepsis. The predictive properties of HBP were compared to C-reactive protein (CRP) and white blood cell count (WBC).Results: Median Injury Severity Score was 33, one-third of the trauma patients received massive transfusion and a quarter was in shock on arrival. Overall 30-day mortality was 8%. Plasma HBP was significantly higher in severely injured patients and associated with shock on arrival, massive transfusions and organ failure. Septic patients had higher levels of HBP only on day 5. When evaluated for prediction of onset of sepsis during the two following days after plasma sampling by receiver operating characteristic (ROC) analyses, areas under the curves were non-significant for all time points. Similar patterns were seen for CRP and WBC.Conclusion: In trauma patients, HBP levels are related to severity of injury and organ dysfunction. Heparin-binding protein was weakly associated with sepsis and only at the later stage of the observation period of 1 week. Moreover, HBP showed poor discriminatory properties as an early biomarker of post-injury sepsis. Trauma-induced inflammation during the post-injury phase may blunt the sepsis-predictive performance of HBP. [ABSTRACT FROM AUTHOR]

Published

2018

2. Heparin-binding protein as a biomarker of acute kidney injury in critical illness.

Author

Tydén, J., Herwald, H., Hultin, M., Walldén, J., Johansson, J., Tydén, J, and Walldén, J

Subjects

KIDNEY injuries, BIOMARKERS, HEPARIN, CATASTROPHIC illness, ISCHEMIA, ACUTE kidney failure, BLOOD proteins, CARRIER proteins, CRITICAL care medicine, LONGITUDINAL method, PEPTIDES, DIAGNOSIS

Abstract

Background: There is no biomarker with high sensitivity and specificity for the development of acute kidney injury (AKI) in a mixed intensive care unit (ICU) population. Heparin-binding protein (HBP) is released from granulocytes and causes increased vascular permeability which plays a role in the development of AKI in sepsis and ischemia. The aim of this study was to investigate whether plasma levels of HBP on admission can predict the development of AKI in a mixed ICU population and in the subgroup with sepsis.Methods: Longitudinal observational study with plasma HBP levels from 245 patients taken on admission to ICU. Presence and severity of AKI was scored daily for 1 week.Results: Mean (95% CI) plasma concentrations of log HBP (ng/ml) in the groups developing different stages of AKI were: stage 0 (n = 175), 3.5 (3.4-3.7); stage 1 (n = 33), 3.7 (3.5-4.0), stage 2 (n = 20), 4.4 (3.5-4.8); and stage 3 (n = 17), 4.6 (3.8-5.2). HBP levels were significantly higher in patients developing AKI stage 3 (P < 0.01) compared to AKI stage 0 and 1. The area under the curve (AUC) for HBP to discriminate the group developing AKI stage 2-3 was 0.70 (CI: 0.58-0.82) and in the subgroup with severe sepsis 0.88 (CI: 0.77-0.99).Conclusion: Heparin-binding protein levels on admission to ICU are associated with the development of severe kidney injury. The relationship between HBP and AKI needs to be further validated in larger studies. [ABSTRACT FROM AUTHOR]

Published

2017

3. Human endogenous peptide p33 inhibits detrimental effects of LL-37 on osteoblast viability.

Author

Svensson, D., Westman, J., Wickström, C., Jönsson, D., Herwald, H., and Nilsson, B.‐O.

Subjects

PEPTIDES, OSTEOBLASTS, ACADEMIC medical centers, ANTI-infective agents, CALCIUM, INTERLEUKINS, RESEARCH funding, WESTERN immunoblotting, CHEMICAL inhibitors, PHYSIOLOGY

Abstract

Background and Objective High levels of the antimicrobial peptide, LL-37, are detected in gingival crevicular fluid from patients with chronic periodontitis. LL-37 not only shows antimicrobial activity but also affects host-cell viability. The objective of the present study was to identify endogenous mechanisms that antagonize the detrimental effects of LL-37 on osteoblast viability, focusing on the human peptide p33 expressed on the surface of various cell types. Material and Methods Human osteoblast-like MG63 cells and human h FOB1.19 osteoblasts were treated with or without LL-37 in the presence or absence of p33. Recombinant human p33 was expressed in an Escherichia coli expression system. Lactate dehydrogenase ( LDH) was assessed using an enzymatic spectrophotometric assay. DNA synthesis was determined by measuring [3 H]-thymidine incorporation. Cell number was assessed by counting cells in a Bürker chamber. Intracellular Ca2+ was monitored by recording Fluo 4- AM fluorescence using a laser scanning confocal microscope. Cellular expression of p33 was determined by western blotting. Results LL-37 caused a concentration-dependent release of LDH from human osteoblasts, showing a half-maximal response value ( EC50) of 4 μ m and a rapid and sustained rise in the intracellular Ca2+ concentration of osteoblasts, suggesting that LL-37 forms pores in the cell membrane. p33 (10 μ m) inhibited the LL-37-induced LDH release and LL-37-evoked rise in intracellular Ca2+ concentration, suggesting that p33 prevents LL-37-induced permeabilization of the cell membrane. Moreover, p33 blocked LL-37-induced attenuation of osteoblast numbers. Also, mucin antagonized, at concentrations representative for nonstimulated whole saliva, LL-37-evoked LDH release, whilst cationic endogenous polyamines had no impact on LL-37-induced LDH release from osteoblasts. Conclusions The endogenous peptide p33 prevents LL-37-induced reduction of human osteoblast viability. Importantly, this mechanism may protect the osteoblasts from LL-37-induced cell damage in patients suffering from chronic periodontitis associated with high levels of LL-37 locally. [ABSTRACT FROM AUTHOR]

Published

2015

4. Heparin-binding protein (HBP/CAP37) - a link to endothelin-1 in endotoxemia-induced pulmonary oedema?

Author

Persson, B P, Halldorsdottir, H, Lindbom, L, Rossi, P, Herwald, H, Weitzberg, E, and Oldner, A

Abstract

Background: Vascular leakage and oedema formation are key components in sepsis. In septic patients, plasma levels of the vasoconstrictive and pro-inflammatory peptide endothelin-1 (ET-1) correlate with mortality. During sepsis, neutrophils release heparin-binding protein (HBP) known to increase vascular permeability and to be a promising biomarker of human sepsis. As disruption of ET-signalling in endotoxemia attenuates formation of oedema, we hypothesized that this effect could be related to decreased levels of HBP. To investigate this, we studied the effects of ET-receptor antagonism on plasma HBP and oedema formation in a porcine model of sepsis. In addition, to further characterize a potential endothelin/HBP interaction, we investigated the effects of graded ET-receptor agonist infusions.Methods: Sixteen anesthetized pigs were subjected to 5 h of endotoxemia and were randomized to receive either the ET-receptor antagonist tezosentan or vehicle after 2 h. Haemodynamics, gas-exchange and lung water were monitored. In separate experiments, plasma HBP was measured in eight non-endotoxemic animals exposed to graded infusion of ET-1 or sarafotoxin 6c.Results: Endotoxemia increased plasma ET-1, plasma HBP, and extravascular lung water. Tezosentan-treatment markedly attenuated plasma HBP and extravascular lung water, and these parameters correlated significantly. Tezosentan decreased pulmonary vascular resistance and increased respiratory compliance. In non-endotoxemic pigs graded ET-1 and sarafotoxin 6c infusions caused a dose-dependent increase in plasma HBP.Conclusions: ET-receptor antagonism reduces porcine endotoxin-induced pulmonary oedema and plasma levels of the oedema-promoting protein HBP. Moreover, direct ET-receptor stimulation distinctively increases plasma HBP. Together, these results suggest a novel mechanism by which ET-1 contributes to formation of oedema during experimental sepsis. [ABSTRACT FROM AUTHOR]

Published

2014

5. Heparin-binding protein ( HBP/ CAP37) - a link to endothelin-1 in endotoxemia-induced pulmonary oedema?

Author

PERSSON, B. P., HALLDORSDOTTIR, H., LINDBOM, L., ROSSI, P., HERWALD, H., WEITZBERG, E., and OLDNER, A.

Subjects

EDEMA, SEPSIS, CARRIER proteins, HEPARIN, NEUTROPHILS, BIOMARKERS, ENDOTOXEMIA, PATIENTS

Abstract

Background Vascular leakage and oedema formation are key components in sepsis. In septic patients, plasma levels of the vasoconstrictive and pro-inflammatory peptide endothelin-1 ( ET-1) correlate with mortality. During sepsis, neutrophils release heparin-binding protein ( HBP) known to increase vascular permeability and to be a promising biomarker of human sepsis. As disruption of ET-signalling in endotoxemia attenuates formation of oedema, we hypothesized that this effect could be related to decreased levels of HBP. To investigate this, we studied the effects of ET-receptor antagonism on plasma HBP and oedema formation in a porcine model of sepsis. In addition, to further characterize a potential endothelin/ HBP interaction, we investigated the effects of graded ET-receptor agonist infusions. Methods Sixteen anesthetized pigs were subjected to 5 h of endotoxemia and were randomized to receive either the ET-receptor antagonist tezosentan or vehicle after 2 h. Haemodynamics, gas-exchange and lung water were monitored. In separate experiments, plasma HBP was measured in eight non-endotoxemic animals exposed to graded infusion of ET-1 or sarafotoxin 6 c. Results Endotoxemia increased plasma ET-1, plasma HBP, and extravascular lung water. Tezosentan-treatment markedly attenuated plasma HBP and extravascular lung water, and these parameters correlated significantly. Tezosentan decreased pulmonary vascular resistance and increased respiratory compliance. In non-endotoxemic pigs graded ET-1 and sarafotoxin 6 c infusions caused a dose-dependent increase in plasma HBP. Conclusions ET-receptor antagonism reduces porcine endotoxin-induced pulmonary oedema and plasma levels of the oedema-promoting protein HBP. Moreover, direct ET-receptor stimulation distinctively increases plasma HBP. Together, these results suggest a novel mechanism by which ET-1 contributes to formation of oedema during experimental sepsis. [ABSTRACT FROM AUTHOR]

Published

2014

6. Heparin-binding protein (HBP): an early marker of respiratory failure after trauma?

Author

Johansson, J, Brattström, O, Sjöberg, F, Lindbom, L, Herwald, H, Weitzberg, E, and Oldner, A

Published

2013

7. Heparin-binding protein ( HBP): an early marker of respiratory failure after trauma?

Author

JOHANSSON, J., BRATTSTRÖM, O., SJÖBERG, F., LINDBOM, L., HERWALD, H., WEITZBERG, E., and OLDNER, A.

Subjects

HEPARIN, CARRIER proteins, RESPIRATORY insufficiency, NEUTROPHILS, MULTIPLE organ failure

Abstract

Background Trauma and its complications contribute to morbidity and mortality in the general population. Trauma victims are susceptible to acute respiratory distress syndrome ( ARDS) and sepsis. Polymorphonuclear leucocytes ( PMNs) are activated after trauma and there is substantial evidence of their involvement in the development of ARDS. Activated PMNs release heparin-binding protein ( HBP), a granule protein previously shown to be involved in acute inflammatory reactions. We hypothesised that there is an increase in plasma HBP content after trauma and that the increased levels are related to the severity of the trauma or later development of severe sepsis and organ failure ( ARDS). Methods and Material We investigated HBP in plasma samples within 36 h from trauma in 47 patients admitted to a level one trauma centre with a mean injury severity score ( ISS) of 26 (21-34). ISS, admission sequential organ failure assessment ( SOFA) and Acute Physiology and Chronic Health Evaluation ( APACHE) II scores were recorded at admission. ARDS and presence of severe sepsis were determined daily during intensive care. Results We found no correlation between individual maximal plasma HBP levels at admission and ISS, admission SOFA or APACHE II. We found, however, a correlation between HBP levels and development of ARDS ( P = 0.026, n = 47), but not to severe sepsis. Conclusion HBP is a potential biomarker candidate for early detection of ARDS development after trauma. Further research is required to confirm a casual relationship between plasma HBP and the development of ARDS. [ABSTRACT FROM AUTHOR]

Published

2013

8. Evaluation of potential biomarkers for the discrimination of bacterial and viral infections.

Author

Chalupa, P., Beran, O., Herwald, H., Kaspříková, N., and Holub, M.

Subjects

DIAGNOSIS of bacterial diseases, VIRAL disease diagnosis, ANALYSIS of variance, BACTERIAL diseases, BIOMARKERS, CALCITONIN, LONGITUDINAL method, PYELONEPHRITIS, RESEARCH funding, STATISTICAL hypothesis testing, STATISTICS, U-statistics, VIRUS diseases, DATA analysis, COMMUNITY-acquired pneumonia, RECEIVER operating characteristic curves, DATA analysis software

Abstract

Purpose: Timely knowledge of the bacterial etiology and localization of infection are important for empirical antibiotic therapy. Thus, the goal of this study was to evaluate routinely used biomarkers together with novel laboratory parameters in the diagnosis of infection. Methods: In this prospective study, 54 adult patients with bacterial infections admitted to the Department of Infectious Diseases were included. For comparison, 27 patients with viral infections were enrolled. In these patients, white blood cell (WBC) counts, differential blood counts, serum levels of procalcitonin (PCT), IL-1β, IL-6, IL-8, IL-10, IL-12, TNF-α, IFN-γ, soluble CD14 (sCD14), heparin-binding protein (HBP), cortisol (Cort), and monocyte surface expression of TLR2, TLR4, HLA-DR, and CD14 were analyzed. Also, these biomarkers were evaluated in 21 patients with acute community-acquired bacterial pneumonia (CABP), as well as in 21 patients with pyelonephritis and urosepsis. Results: The highest sensitivity and specificity (expressed as the area under the curve [AUC]) for bacterial infection were observed in serum concentration of PCT (0.952), neutrophil and lymphocyte counts (0.852 and 0.841, respectively), and serum levels of HBP (0.837), IL-6 (0.830), and Cort (0.817). In addition, the serum levels of IFN-γ and Cort were significantly higher and IL-8 levels were lower in CABP when compared to pyelonephritis or urosepsis. Conclusions: From the novel potential biomarkers, only PCT demonstrated superiority over the routine parameters in the differentiation of bacterial from viral infections. However, some of the novel parameters should be further evaluated in larger and better characterized cohorts of patients in order to find their clinical applications. [ABSTRACT FROM AUTHOR]

Published

2011

9. Modulation of Membrane Traffic by Microorganisms.

Author

Tapper, H. and Herwald, H.

Published

2003

10. Innate immunity - a clinical perspective.

Author

Egesten, A., Gordon, S., and Herwald, H.

Subjects

NATURAL immunity

Abstract

Content List ‐ 15th Key symposium ‐ "Innate immunity". [ABSTRACT FROM AUTHOR]

Published

2019

11. Heparin-binding protein in ventilator-induced lung injury.

Author

Tydén, Jonas, Larsson, N., Lehtipalo, S., Herwald, H., Hultin, M., Walldén, J., Behndig, A. F., and Johansson, J.

Subjects

HEPARIN, CARRIER proteins, LUNG injury treatment, VENTILATION, GRANULOCYTES

Abstract

Background: Although mechanical ventilation is often lifesaving, it can also cause injury to the lungs. The lung injury is caused by not only high pressure and mechanical forces but also by inflammatory processes that are not fully understood. Heparin-binding protein (HBP), released by activated granulocytes, has been indicated as a possible mediator of increased vascular permeability in the lung injury associated with trauma and sepsis. We investigated if HBP levels were increased in the bronchoalveolar lavage fluid (BALF) or plasma in a pig model of ventilator-induced lung injury (VILI). We also investigated if HBP was present in BALF from healthy volunteers and in intubated patients in the intensive care unit (ICU).Methods: Anaesthetized pigs were randomized to receive ventilation with either tidal volumes of 8 ml/kg (controls, n = 6) or 20 ml/kg (VILI group, n = 6). Plasma and BALF samples were taken at 0, 1, 2, 4, and 6 h. In humans, HBP levels in BALF were sampled from 16 healthy volunteers and from 10 intubated patients being cared for in the ICU.Results: Plasma levels of HBP did not differ between pigs in the control and VILI groups. The median HBP levels in BALF were higher in the VILI group after 6 h of ventilation compared to those in the controls (1144 ng/ml (IQR 359-1636 ng/ml) versus 89 ng/ml (IQR 33-191 ng/ml) ng/ml, respectively, p = 0.02).The median HBP level in BALF from healthy volunteers was 0.90 ng/ml (IQR 0.79-1.01 ng/ml) as compared to 1959 ng/ml (IQR 612-3306 ng/ml) from intubated ICU patients (p < 0.001).Conclusions: In a model of VILI in pigs, levels of HBP in BALF increased over time compared to controls, while plasma levels did not differ between the two groups.HBP in BALF was high in intubated ICU patients in spite of the seemingly non-harmful ventilation, suggesting that inflammation from other causes might increase HBP levels. [ABSTRACT FROM AUTHOR]

Published

2018

12. Heparin binding protein interacts with endothelial cell proteoglycans and the binding protein for complement factor lq and H-kininogen.

Author

Olofsson, A M, Herwald, H, Flodgaard, H, and Lundgren-Åkerlund, E

Published

1997