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1. Potent Trivalent Inhibitors of Thrombin through Hybridization of Salivary Sulfopeptides from Hematophagous Arthropods

Author

Mike C. L. Wu, Imala Alwis, Richard J. Payne, Pedro Pereira, Shaun P. Jackson, Emma E. Watson, Jorge Ripoll-Rozada, Stijn M. Agten, Luke J. Dowman, Biochemie, and RS: Carim - B01 Blood proteins & engineering

Subjects
Male, Proteases, Tsetse Flies, protein synthesis, medicine.medical_treatment, Protein Engineering, 010402 general chemistry, 01 natural sciences, Catalysis, Thrombin, Amblyomma, Catalytic Domain, Anopheles, medicine, Animals, Humans, Salivary Proteins and Peptides, Protease, biology, 010405 organic chemistry, Chemistry, anticoagulant, Rational design, Anticoagulants, Active site, Thrombosis, General Chemistry, Native chemical ligation, 0104 chemical sciences, Mice, Inbred C57BL, Coagulation, Biochemistry, peptide ligation, biology.protein, peptide engineering, Platelet Aggregation Inhibitors, Protein Binding, medicine.drug, Discovery and development of direct thrombin inhibitors
Abstract

Blood feeding arthropods, such as leeches, ticks, flies and mosquitoes, provide a privileged source of peptidic anticoagulant molecules. These primarily operate through inhibition of the central coagulation protease thrombin by binding to the active site and either exosite I or exosite II. Herein, we describe the rational design of a novel class of trivalent thrombin inhibitors that simultaneously block both exosites as well as the active site. These engineered hybrids were synthesized using tandem diselenide-selenoester ligation (DSL) and native chemical ligation (NCL) reactions in one-pot. The most potent trivalent inhibitors possessed femtomolar inhibition constants against alpha-thrombin and were selective over related coagulation proteases. A lead hybrid inhibitor possessed potent anticoagulant activity, blockade of both thrombin generation and platelet aggregation in vitro and efficacy in a murine thrombosis model at 1 mg kg(-1). The rational engineering approach described here lays the foundation for the development of potent and selective inhibitors for a range of other enzymatic targets that possess multiple sites for the disruption of protein-protein interactions, in addition to an active site.

Published
2021
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3. Rapid assembly and profiling of an anticoagulant sulfoprotein library

Author

Ashley Lee, Tim Pasch, Charlotte Franck, Shaun P. Jackson, Emma E. Watson, Jessica Sayers, Bhavesh Premdjee, Pedro M. Martins, Pedro Pereira, Jorge Ripoll-Rozada, Richard J. Payne, Mike C. L. Wu, and Maria Filipa Pinto

Subjects
medicine.drug_class, Peptide, Serine, Structure-Activity Relationship, Sulfation, Thrombin, medicine, Humans, Amino Acid Sequence, Salivary Proteins and Peptides, Tyrosine, Blood Coagulation, Peptide sequence, Gene Library, chemistry.chemical_classification, Multidisciplinary, Chemistry, Biomolecule, Anticoagulant, Anticoagulants, Computational Biology, Biochemistry, Physical Sciences, Insect Proteins, Protein Processing, Post-Translational, medicine.drug
Abstract

Hematophagous organisms produce a suite of salivary proteins which interact with the host's coagulation machinery to facilitate the acquisition and digestion of a bloodmeal. Many of these biomolecules inhibit the central blood-clotting serine proteinase thrombin that is also the target of several clinically approved anticoagulants. Here a bioinformatics approach is used to identify seven tick proteins with putative thrombin inhibitory activity that we predict to be posttranslationally sulfated at two conserved tyrosine residues. To corroborate the biological role of these molecules and investigate the effects of amino acid sequence and sulfation modifications on thrombin inhibition and anticoagulant activity, a library of 34 homogeneously sulfated protein variants were rapidly assembled using one-pot diselenide-selenoester ligation (DSL)-deselenization chemistry. Downstream functional characterization validated the thrombin-directed activity of all target molecules and revealed that posttranslational sulfation of specific tyrosine residues crucially modulates potency. Importantly, access to this homogeneously modified protein library not only enabled the determination of key structure-activity relationships and the identification of potent anticoagulant leads, but also revealed subtleties in the mechanism of thrombin inhibition, between and within the families, that would be impossible to predict from the amino acid sequence alone. The synthetic platform described here therefore serves as a highly valuable tool for the generation and thorough characterization of libraries of related peptide and/or protein molecules (with or without modifications) for the identification of lead candidates for medicinal chemistry programs.

Published
2019
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4. Absence of the C5a Receptor C5aR2 Worsens Ischemic Tissue Injury by Increasing C5aR1-Mediated Neutrophil Infiltration

Author

Trent M. Woodruff, Mike C. L. Wu, John D. Lee, and Marc J. Ruitenberg

Subjects
Male, Immunology, Complement C5a, Complement factor I, C5a receptor, Proinflammatory cytokine, Mice, medicine, Immunology and Allergy, Animals, Humans, Receptor, Receptor, Anaphylatoxin C5a, Mice, Knockout, business.industry, medicine.disease, Pathophysiology, Disease Models, Animal, medicine.anatomical_structure, Jejunum, Tissue ischemia, Neutrophil Infiltration, Mesenteric Ischemia, Reperfusion Injury, Bone marrow, business, Infiltration (medical)
Abstract

Neutrophil infiltration to ischemic tissues following reperfusion worsens injury. A key driver of neutrophil recruitment and activation is the complement factor C5a, which signals through two receptors, C5aR1 and C5aR2. In this study, we used a neutrophil-dependent mouse model of intestinal ischemia-reperfusion (IR) injury to investigate the underexplored role of C5aR2 in neutrophil mobilization, recruitment, and disease outcomes. We show that intestinal IR induces rapid neutrophil mobilization along with a concomitant reduction in plasma C5a levels that is driven by both C5aR1 and C5aR2. Intestinal IR in C5aR2−/− mice led to worsened intestinal damage and increased neutrophil infiltration. Inhibition of C5aR1 signaling in C5aR2−/− mice with PMX53 prevented neutrophil accumulation and reduced IR pathology, suggesting a key requirement for enhanced neutrophil C5aR1 activation in the absence of C5aR2 signaling. Interestingly, C5aR2 deficiency also reduced circulating neutrophil numbers after IR, as well as following G-CSF–mediated bone marrow mobilization, which was independent of C5aR1, demonstrating that C5aR2 has unique and distinct functions from C5aR1 in neutrophil egress. Despite enhanced tissue injury in C5aR2−/− IR mice, there were significant reductions in intestinal proinflammatory cytokines, highlighting complicated dual protective/pathogenic roles for C5aR2 in pathophysiology. Collectively, we show that C5aR2 is protective in intestinal IR by inhibiting C5aR1-mediated neutrophil recruitment to the ischemic tissue. This is despite the potentially local pathogenic effects of C5aR2 in increasing intestinal proinflammatory cytokines and enhancing circulating neutrophil numbers in response to mobilizing signals. Our data therefore suggest that this balance between the dual pro- and anti-inflammatory roles of C5aR2 ultimately dictates disease outcomes.

Published
2020

5. Acetate protects against intestinal ischemia-reperfusion injury independent of its cognate free fatty acid 2 receptor

Author

Mike C. L. Wu, Trent M. Woodruff, Philip M. Hansbro, Zoe Schofield, and Mark E. Cooper

Subjects
0301 basic medicine, Male, Neutrophils, Ischemia, Pharmacology, Acetates, Biochemistry, Receptors, G-Protein-Coupled, 03 medical and health sciences, Mice, 0302 clinical medicine, medicine.artery, Genetics, medicine, Animals, cardiovascular diseases, Superior mesenteric artery, Receptor, Molecular Biology, chemistry.chemical_classification, Chemistry, Intestinal ischemia, Fatty acid, medicine.disease, Ligand (biochemistry), Intestines, Mice, Inbred C57BL, 030104 developmental biology, Neutrophil Infiltration, Reperfusion Injury, Infiltration (medical), Reperfusion injury, 030217 neurology & neurosurgery, Biotechnology
Abstract

Free fatty acid 2 receptor (FFA2) is highly expressed on neutrophils and, when activated by its cognate ligand acetate, generates potent anti-inflammatory activities. The roles of FFA2 and acetate have not been explored in ischemia-reperfusion injury (IRI). We therefore examined the function of FFA2 and the therapeutic potential of acetate to reduce tissue injury in an acute model of intestinal IRI. The superior mesenteric artery of wild-type (WT) and FFA2-/- mice was briefly occluded then reperfused following treatment with acetate or vehicle. The absence of FFA2 resulted in intestinal injury similar to that observed in WT mice, indicating a minimal causal role for FFA2 in this model. Acetate treatment to WT mice prior to ischemia profoundly protected the intestine from IRI-induced damage. Amelioration of IRI was also observed, although to a lesser extent, when acetate was administered to FFA2-/- mice demonstrating that certain protective effects of acetate were FFA2-independent. Remarkably, despite the lack of tissue damage following IRI, acetate-treated mice had markedly increased neutrophil infiltration to the reperfused intestine which was dependent on FFA2. These studies reveal a minimal causal role for FFA2 in intestinal IRI but highlight the novel therapeutic potential for acetate in the amelioration of ischemia-mediated tissue damage.

Published
2020

6. Thromboinflammatory Functions of Platelets in Ischemia–Reperfusion Injury and Its Dysregulation in Diabetes

Author

Yuping Yuan, Mike C. L. Wu, Sophie Maiocchi, Imala Alwis, and Shaun P. Jackson

Subjects
Blood Platelets, 0301 basic medicine, medicine.medical_specialty, Ischemia, Inflammation, Context (language use), 030204 cardiovascular system & hematology, 03 medical and health sciences, 0302 clinical medicine, Internal medicine, Diabetes mellitus, Diabetes Mellitus, Humans, Medicine, Platelet, Endothelial dysfunction, business.industry, Thrombosis, Hematology, medicine.disease, 030104 developmental biology, Reperfusion Injury, Cardiology, medicine.symptom, Cardiology and Cardiovascular Medicine, business, Reperfusion injury
Abstract

Ischemia–reperfusion (IR) injury is a common complication of a variety of cardiovascular diseases, including ischemic stroke and myocardial infarction (MI). While timely re-establishment of blood flow in a thrombosed artery is the primary goal of acute therapy in these diseases, paradoxically, reperfusion of ischemic tissue can cause widespread microvascular dysfunction that significantly exacerbates organ damage. Reperfusion injury is associated with activation of the humoral and cellular components of the hemostatic and innate immune systems and also with excessive reactive oxygen species production, endothelial dysfunction, thrombosis, and inflammation. Platelets are critical mediators of thromboinflammation during reperfusion injury and a hyperactive platelet phenotype may contribute to an exaggerated IR injury response. This is particularly relevant to diabetes which is characteristically associated with hyperactive platelets, significantly worse IR injury, increased organ damage, and increased risk of death. However, the mechanisms underlying vulnerability to IR injury in diabetic individuals is not well defined, nor the role of “diabetic platelets” in this process. This review summarizes recent progress in understanding the role of platelets in promoting microvascular dysfunction and inflammation in the context of IR injury. Furthermore, the authors discuss aspects of the thromboinflammatory function of platelets that are dysregulated in diabetes. They conclude that diabetes likely enhances the capacity of platelets to mediate microvascular thrombosis and inflammation during IR injury, which has potentially important implications for the future design of antiplatelet agents that can reduce microvascular dysfunction and inflammation.

Published
2018
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9. Multi-photon near-infrared emission saturation nanoscopy using upconversion nanoparticles

Author

Mehran Kianinia, Dayong Jin, Baoming Wang, Xuchen Shan, Qian Peter Su, Shaun P. Jackson, Chaohao Chen, Peng Xi, Fan Wang, Mike C. L. Wu, Shihui Wen, Milos Toth, Yongtao Liu, Du Li, and Igor Aharonovich

Subjects
Materials science, Photon, Science, General Physics and Astronomy, 02 engineering and technology, 010402 general chemistry, 01 natural sciences, Article, General Biochemistry, Genetics and Molecular Biology, law.invention, law, Stimulated emission, lcsh:Science, Penetration depth, Multidisciplinary, business.industry, Near-infrared spectroscopy, STED microscopy, General Chemistry, 021001 nanoscience & nanotechnology, Laser, 0104 chemical sciences, Femtosecond, Optoelectronics, lcsh:Q, 0210 nano-technology, business, Excitation
Abstract

Multiphoton fluorescence microscopy (MPM), using near infrared excitation light, provides increased penetration depth, decreased detection background, and reduced phototoxicity. Using stimulated emission depletion (STED) approach, MPM can bypass the diffraction limitation, but it requires both spatial alignment and temporal synchronization of high power (femtosecond) lasers, which is limited by the inefficiency of the probes. Here, we report that upconversion nanoparticles (UCNPs) can unlock a new mode of near-infrared emission saturation (NIRES) nanoscopy for deep tissue super-resolution imaging with excitation intensity several orders of magnitude lower than that required by conventional MPM dyes. Using a doughnut beam excitation from a 980 nm diode laser and detecting at 800 nm, we achieve a resolution of sub 50 nm, 1/20th of the excitation wavelength, in imaging of single UCNP through 93 μm thick liver tissue. This method offers a simple solution for deep tissue super resolution imaging and single molecule tracking., Upconversion nanoparticles offer the potential for deep tissue biological imaging. Here, Chen et al. develop super resolution optical imaging in the near-infrared for imaging with sub-50 nm resolution through almost 100 microns of tissue.

Published
2018
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10. Neutrophil macroaggregates promote widespread pulmonary thrombosis after gut ischemia

Author

Simone M. Schoenwaelder, Benjamin T. Kile, David Bark, Zane Kaplan, James D. McFadyen, Emma C. Josefsson, Imala Alwis, Mike C. L. Wu, Shaun P. Jackson, Yuping Yuan, Alan Pham, and Katrina J. Ashworth

Subjects
Blood Platelets, 0301 basic medicine, Pathology, medicine.medical_specialty, Neutrophils, Ischemia, Phosphatidylserines, Biology, Cyclophilins, 03 medical and health sciences, medicine, Animals, Humans, Platelet, Splanchnic Circulation, Platelet activation, Lung, Cell Aggregation, Respiratory Distress Syndrome, Cell Membrane, Thrombosis, General Medicine, medicine.disease, Cell aggregation, Gastrointestinal Tract, Mice, Inbred C57BL, 030104 developmental biology, medicine.anatomical_structure, Immunology, Reperfusion injury, Cyclophilin D, Intravital microscopy
Abstract

Gut ischemia is common in critically ill patients, promoting thrombosis and inflammation in distant organs. The mechanisms linking hemodynamic changes in the gut to remote organ thrombosis remain ill-defined. We demonstrate that gut ischemia in the mouse induces a distinct pulmonary thrombotic disorder triggered by neutrophil macroaggregates. These neutrophil aggregates lead to widespread occlusion of pulmonary arteries, veins, and the microvasculature. A similar pulmonary neutrophil-rich thrombotic response occurred in humans with the acute respiratory distress syndrome. Intravital microscopy during gut ischemia-reperfusion injury revealed that rolling neutrophils extract large membrane fragments from remnant dying platelets in multiple organs. These platelet fragments bridge adjacent neutrophils to facilitate macroaggregation. Platelet-specific deletion of cyclophilin D, a mitochondrial regulator of cell necrosis, prevented neutrophil macroaggregation and pulmonary thrombosis. Our studies demonstrate the existence of a distinct pulmonary thrombotic disorder triggered by dying platelets and neutrophil macroaggregates. Therapeutic targeting of platelet death pathways may reduce pulmonary thrombosis in critically ill patients.

Published
2017
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11. C5L2: a controversial receptor of complement anaphylatoxin, C5a

Author

Mike C. L. Wu, Rui Li, Stephen M. Taylor, Trent M. Woodruff, and Liam G. Coulthard

Subjects
Arrestins, Complement C5a, Biology, Biochemistry, C5a receptor, Proinflammatory cytokine, 03 medical and health sciences, 0302 clinical medicine, Sepsis, Genetics, Animals, Humans, Anaphylatoxin, Receptor, Anaphylatoxin C5a, Molecular Biology, beta-Arrestins, 030304 developmental biology, 0303 health sciences, Beta-Arrestins, Protein Structure, Tertiary, Receptors, Complement, Complement system, Disease Models, Animal, Gene Expression Regulation, GPR77, Immunology, Receptors, Chemokine, Signal transduction, Neuroscience, Signal Transduction, 030215 immunology, Biotechnology
Abstract

C5a is the paramount proinflammatory mediator of the complement cascade, and has been previously thought to act only through a single, G-protein-coupled, C5a receptor (C5aR; also termed CD88). In 2000, a second C5a receptor, C5L2 (previously known as GPR77), was discovered; yet, despite 12 yr of intensive research, its biological, or pathophysiological, function is both enigmatic and controversial. Unlike C5aR, this receptor does not couple to G proteins, and early studies promoted the hypothesis that C5L2 functions as a decoy receptor. However, recent data have provided other evidence for more complicated and conflicting interactions between C5L2 and other inflammatory mediators. C5L2 has been recently demonstrated to physically interact with both C5aR and β-arrestin to negatively regulate C5aR signaling toward an anti-inflammatory manner, and to reduce pathology, in several disease models in vivo. In direct contrast, other groups have demonstrated that C5L2 stimulation caused release of HMGB1 both in vitro and in vivo, and enhanced pathology in sepsis models, suggesting a clear proinflammatory signaling role. These astoundingly contradictory data challenge our precepts and complicate the foundational bases for the possible targeting of C5L2 as a therapeutic option in inflammatory disease. C5L2 may be the great masquerader in complement biology; its function dependent on the cell type, species, and disease context. Because of these unusual and unforeseen complexities, we present the current state of knowledge on C5L2 structure, expression and, most controversially, its putative functions.-Li, R., Coulthard, L.G., Wu, M. C. L., Taylor, S. M., Woodruff, T. M. C5L2: a controversial receptor of complement anaphylatoxin, C5a.

Published
2012
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12. Inhibition of Inflammation and Fibrosis by a Complement C5a Receptor Antagonist in DOCA-Salt Hypertensive Rats

Author

Robert Reid, Trent M. Woodruff, Lindsay Brown, Con Stylianou, Stephen M. Taylor, David P. Fairlie, Abishek Iyer, and Mike C. L. Wu

Subjects
Male, Nitroprusside, medicine.medical_specialty, Cardiac fibrosis, Heart Ventricles, Gene Expression, Aorta, Thoracic, Blood Pressure, Inflammation, Peptides, Cyclic, Cicatrix, Norepinephrine, Fibrosis, Coronary Circulation, Internal medicine, Ventricular Dysfunction, Animals, Medicine, Mast Cells, Cardiac Output, Rats, Wistar, Endothelial dysfunction, Desoxycorticosterone, Ventricular remodeling, Receptor, Anaphylatoxin C5a, Pharmacology, business.industry, Myocardium, Heart, Endomyocardial Fibrosis, medicine.disease, Leukocyte extravasation, Acetylcholine, Rats, Complement system, Vasodilation, Endocrinology, Echocardiography, Vasoconstriction, Hypertension, Leukocytes, Mononuclear, Hypertrophy, Left Ventricular, Collagen, medicine.symptom, Cardiology and Cardiovascular Medicine, business, Infiltration (medical)
Abstract

The anaphylatoxin C5a generated by activation of the innate immunity complement system is a potent inflammatory peptide mediator through the G-protein-coupled receptor C5aR (CD88) present in immune-inflammatory cells, including monocytes, macrophages, neutrophils, T cells, and mast cells. Inflammatory cells infiltrate and initiate the development of fibrosis in the chronically hypertensive heart. In this study, we have investigated whether treatment with a selective C5aR antagonist prevents cardiovascular remodeling in deoxycorticosterone acetate (DOCA)-salt hypertensive rats. Control and DOCA-salt rats were treated with PMX53 (AcF-[OPdChaWR], 1 mg·kg·d oral gavage) for 32 days; structural and functional changes in cardiovascular system were determined. DOCA-salt hypertension increased leukocyte extravasation into ventricular tissue, increasing collagen deposition and ventricular stiffness; PMX53 treatment attenuated these changes, thereby improving cardiac function. Further, treatment with PMX53 suppressed an increased expression of C5aR in the left ventricle from DOCA-salt rats, consistent with the reduced infiltration of inflammatory cells. Vascular endothelial dysfunction in thoracic aortic rings was attenuated by PMX53 treatment, but systolic blood pressure was unchanged in DOCA-salt rats. In the heart, PMX53 treatment attenuated inflammatory cell infiltration, fibrosis, and ventricular stiffness, indicating that C5aR is critically involved in ventricular remodeling by regulating inflammatory responses in the hypertensive heart.

Published
2011
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13. EPHA4-FC TREATMENT REDUCES ISCHEMIA/REPERFUSION-INDUCED INTESTINAL INJURY BY INHIBITING VASCULAR PERMEABILITY

Author

Michael M. Morgan, Stephen M. Taylor, Mark G. Coulthard, Nathan T. Bain, Jeffrey Lipman, Mike C. L. Wu, Michael J. Ting, Andrew W. Boyd, Angela Jeanes, and Trent M. Woodruff

Subjects
0301 basic medicine, Male, medicine.medical_treatment, Inflammation, Vascular permeability, Biology, Critical Care and Intensive Care Medicine, Proinflammatory cytokine, Cell Line, Capillary Permeability, 03 medical and health sciences, Mice, medicine, Ephrin, Animals, Humans, Tumor Necrosis Factor-alpha, Erythropoietin-producing hepatocellular (Eph) receptor, Receptor, EphA4, medicine.disease, biological factors, Immunoglobulin Fc Fragments, 030104 developmental biology, Cytokine, Reperfusion Injury, Immunology, Emergency Medicine, Cancer research, Tumor necrosis factor alpha, medicine.symptom, Reperfusion injury, Signal Transduction
Abstract

The inflammatory response is characterized by increased endothelial permeability, which permits the passage of fluid and inflammatory cells into interstitial spaces. The Eph/ephrin receptor ligand system plays a role in inflammation through a signaling cascade, which modifies Rho-GTPase activity. We hypothesized that blocking Eph/ephrin signaling using an EphA4-Fc would result in decreased inflammation and tissue injury in a model of ischemia/reperfusion (I/R) injury. Mice undergoing intestinal I/R pretreated with the EphA4-Fc had significantly reduced intestinal injury compared to mice injected with the control Fc. This reduction in I/R injury was accompanied by significantly reduced neutrophil infiltration, but did not affect intestinal inflammatory cytokine generation. Using microdialysis, we identified that intestinal I/R induced a marked increase in systemic vascular leakage, which was completely abrogated in EphA4-Fc-treated mice. Finally, we confirmed the direct role of Eph/ephrin signaling in endothelial leakage by demonstrating that EphA4-Fc inhibited tumor necrosis factor-[alpha]–induced vascular permeability in human umbilical vein endothelial cells. This study identifies that Eph/ephrin interaction induces proinflammatory signaling in vivo by inducing vascular leak and neutrophil infiltration, which results in tissue injury in intestinal I/R. Therefore, therapeutic targeting of Eph/ephrin interaction using inhibitors, such as EphA4-Fc, may be a novel method to prevent tissue injury in acute inflammation by influencing endothelial integrity and by controlling vascular leak.

Published
2016

14. The Receptor for Advanced Glycation Endproducts Does Not Contribute to Pathology in a Mouse Mesenteric Ischemia/Reperfusion-Induced Injury Model

Author

Susanna Mantovani, Timothy D. Gilmour, Mike C. L. Wu, and Trent M. Woodruff

Subjects
lcsh:Immunologic diseases. Allergy, Pathology, medicine.medical_specialty, Neutrophils, medicine.medical_treatment, ischemia–reperfusion injury, ischemia-reperfusion injury, Immunology, Ischemia, Inflammation, C3a, Rage, 03 medical and health sciences, 0302 clinical medicine, Immune system, Intestinal mucosa, Intestine, Small, medicine, Immunology and Allergy, Receptor, Original Research, HMGB-1, 030304 developmental biology, 0303 health sciences, business.industry, medicine.disease, Small intestine, Cytokine, medicine.anatomical_structure, Mesenteric ischemia, 030220 oncology & carcinogenesis, medicine.symptom, lcsh:RC581-607, business, small intestine, human activities
Abstract

The receptor for advanced glycation endproducts (RAGE) can engage a diverse class of ligands and contribute to the immune and inflammatory response to infection and injury. It is known to be a pathogenic receptor in many inflammatory diseases, including ischemia/reperfusion (IR) injuries in several tissues; however, its role has not been investigated in IR injuries of the intestine to date. Mesenteric (or intestinal) IR leads to recruitment of inflammatory cells into intestinal interstitial spaces, which markedly disrupts intestinal mucosa. IR-induced mucosal injury is accompanied by the development of a local and systemic inflammatory response and remote organ injury, and results in high mortality in the clinic. We hypothesized that elimination of RAGE signaling using RAGE(-/-) mice would result in decreased local and remote organ injury and reduced inflammation in a mesenteric IR model, and thus be a target for therapeutic intervention. We found that RAGE ligands including HMGB-1 and C3a were elevated after mesenteric IR indicating the potential for enhanced RAGE activation in this model. However despite this, wild-type and RAGE(-/-) mice both displayed similar degrees of mesenteric injury, neutrophil infiltration, intestinal edema, cytokine generation, neutrophil mobilization, and remote organ injury after mesenteric IR. We, therefore, conclude that despite its role in other organ IR injuries, and the robust production of RAGE ligands after intestinal ischemia, RAGE itself does not directly influence tissue injury and the inflammatory response in mesenteric IR.

Published
2015
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15. Valproic acid selectively increases vascular endothelial tissue-type plasminogen activator production and reduces thrombus formation in the mouse

Author

Be'eri Niego, Shaun P. Jackson, Maithili Sashindranath, Sverker Jern, Mia Magnusson, Imala Alwis, Mike C. L. Wu, Per Fogelstrand, Robert L. Medcalf, Lars Glise, Niklas Bergh, Maria Daglas, and Pia Larsson

Subjects
Blood Platelets, Male, Platelet Function Tests, medicine.medical_treatment, Hemorrhage, 030204 cardiovascular system & hematology, Pharmacology, Tissue plasminogen activator, Hippocampus, Fibrin, 03 medical and health sciences, Mice, 0302 clinical medicine, In vivo, Fibrinolysis, medicine, Animals, Platelet, RNA, Messenger, Thrombus, Enzyme Inhibitors, Blood Coagulation, Aorta, Microscopy, Confocal, biology, Chemistry, Valproic Acid, Thrombosis, Hematology, medicine.disease, Immunohistochemistry, Mice, Inbred C57BL, Coagulation, Tissue Plasminogen Activator, Immunology, biology.protein, lipids (amino acids, peptides, and proteins), Endothelium, Vascular, Plasminogen activator, 030217 neurology & neurosurgery, medicine.drug
Abstract

Essentials Stimulating endogenous fibrinolysis could be a novel antithrombotic strategy. The effect of valproic acid on endothelial tissue plasminogen activator in mice was investigated. Valproic acid increased tissue plasminogen activator expression in vascular endothelium. Valproic acid reduced fibrin deposition and thrombus formation after vascular injury. SummaryBackground The endogenous fibrinolytic system has rarely been considered as a target to prevent thrombotic disease. Tissue-type plasminogen activator (t-PA) production is potently increased by histone deacetylase (HDAC) inhibitors in endothelial cells in vitro, but whether this translates into increased vascular t-PA production and an enhanced fibrinolytic capacity in vivo is unknown. Objectives To determine whether the HDAC inhibitor valproic acid (VPA) stimulates production of t-PA in the vasculature of mice, and whether VPA pretreatment affects fibrin deposition and clot formation after mechanical vessel injury. Methods Mice were injected with VPA twice daily for up to 5 days. t-PA mRNA, and antigen expression in the mouse aorta and the circulating levels of t-PA were determined. Fibrin and thrombus dynamics after mechanical vessel injury were monitored with intravital confocal microscopy. Potential effects of VPA on platelets and coagulation were investigated. Results and Conclusions We found that VPA treatment increased vascular t-PA production in vivo and, importantly, that VPA administration was associated with reduced fibrin accumulation and smaller thrombi in response to vascular injury, but still was not associated with an increased risk of bleeding. Furthermore, we observed that higher concentrations of VPA were required to stimulate t-PA production in the brain than in the vasculature. Thus, this study shows that VPA can be dosed to selectively manipulate the fibrinolytic system in the vascular compartment and reduce thrombus formation in vivo.

Published
2015

16. Neutrophils--a key component of ischemia-reperfusion injury

Author

Reena Halai, Mark E. Cooper, Trent M. Woodruff, Mike C. L. Wu, and Zoe Schofield

Subjects
Neutrophils, Ischemia, Inflammation, Neutropenia, urologic and male genital diseases, Critical Care and Intensive Care Medicine, Neutrophil Activation, medicine, Animals, Humans, cardiovascular diseases, Myocardial infarction, Molecular Targeted Therapy, Cause of death, urogenital system, business.industry, fungi, medicine.disease, female genital diseases and pregnancy complications, Transplantation, Neutrophil Infiltration, Reperfusion Injury, Immunology, Emergency Medicine, Cytokines, medicine.symptom, business, Infiltration (medical), Reperfusion injury
Abstract

Ischemia-reperfusion injury (IRI) is a common occurrence following myocardial infarction, transplantation, stroke, and trauma that can lead to multiple organ failure, which remains the foremost cause of death in critically ill patients. Current therapeutic strategies for IRI are mainly palliative, and there is an urgent requirement for a therapeutic that could prevent or reverse tissue damage caused by IRI. Neutrophils are the primary responders following ischemia and reperfusion and represent important components in the protracted inflammatory response and severity associated with IRI. Experimental studies demonstrate neutrophil infiltration at the site of ischemia and show that inducing neutropenia can protect organs from IRI. In this review, we highlight the mechanisms involved in neutrophil recruitment, activation, and adherence and how this contributes to disease severity in IRI. Inhibiting neutrophil mobilization, tissue recruitment, and ultimately neutrophil-associated activation of local and systemic inflammatory responses may have therapeutic potential in the amelioration of local and remote tissue damage following IRI.

Published
2013

17. The receptor for complement component C3a mediates protection from intestinal ischemia-reperfusion injuries by inhibiting neutrophil mobilization

Author

Jason P. Lynch, Rick A. Wetsel, Simon Phipps, Mike C. L. Wu, Susanna Mantovani, Marc J. Ruitenberg, Faith H. Brennan, Stephen M. Taylor, and Trent M. Woodruff

Subjects
Agonist, medicine.drug_class, Neutrophils, Complement C5a, Apoptosis, Biology, Granulocyte, Pharmacology, Hemoglobins, Mice, In vivo, medicine, Animals, Receptor, Mice, Knockout, Multidisciplinary, Histological Techniques, Biological Sciences, Complement system, Receptors, Complement, Intestines, medicine.anatomical_structure, Reperfusion Injury, Immunology, Cytokines, Bone marrow, Antagonism
Abstract

C3a is a key complement activation fragment, yet its neutrophil-expressed receptor (C3aR) still has no clearly defined role. In this study, we used a neutrophil-dependent mouse model of intestinal ischemia-reperfusion (IR) injury to explore the role of C3aR in acute tissue injuries. C3aR deficiency worsened intestinal injury, which corresponded with increased numbers of tissue-infiltrating neutrophils. Circulating neutrophils were significantly increased in C3aR −/− mice after intestinal ischemia, and C3aR −/− mice also mobilized more circulating neutrophils after granulocyte colony-stimulating factor infusion compared with WT mice, indicating a specific role for C3aR in constraining neutrophil mobilization in response to intestinal injury. In support of this role, C3aR −/− mice reconstituted with WT bone marrow reversed IR pathology back to WT levels. Complement C5a receptor (C5aR) antagonism in C3aR −/− mice also rectified the worsened pathology after intestinal IR injury but had no effect on circulating neutrophils, highlighting the opposing roles of C3a and C5a in disease pathogenesis. Finally, we found that using a potent C3a agonist to activate C3aR in vivo reduced neutrophil mobilization and ameliorated intestinal IR pathology in WT, but not C3aR −/− , mice. This study identifies a role for C3aR in regulating neutrophil mobilization after acute intestinal injury and highlights C3aR agonism as a potential treatment option for acute, neutrophil-driven pathologies.

Published
2013

19. The role of complement anaphylatoxin receptors in mesenteric ischemia/reperfusion-induced injury

Author

Stephen M. Taylor, Helga D. Manthey, Mike C. L. Wu, Tyson A. Moore, and Trent M. Woodruff

Subjects
business.industry, Anaphylatoxin receptors, Immunology, Ischemia, chemical and pharmacologic phenomena, Inflammation, medicine.disease, Complement system, Complement (complexity), Pathogenesis, Medicine, Anaphylatoxin, medicine.symptom, business, Receptor, Molecular Biology
Abstract

Inflammation is a major driver of pathology in ischemia reperfusion (IR) injuries. The complement activation products complement anaphylatoxin 3a (C3a) and complement anaphylatoxin (C5a), are powerful pro-inflammatory mediators which activate inflammatory cells and the release of pro-inflammatory substances involved in the pathology of IR. We are currently exploring the role of the anaphylatoxin receptors using mice deficient in these receptors (CD88, C5L2, and C3aR). This study demonstrates a role for complement activation, C5a generation and CD88 activation in the pathogenesis of intestinal IR injury in mice.

Published
2010
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