Your search keyword '"Burns AR"' showing total 10 results

1. Platelet and Erythrocyte Extravasation across Inflamed Corneal Venules Depend on CD18, Neutrophils, and Mast Cell Degranulation.

Author

De La Cruz A, Hargrave A, Magadi S, Courson JA, Landry PT, Zhang W, Lam FW, Bray MA, Smith CW, Burns AR, and Rumbaut RE

Subjects

Animals, CD18 Antigens deficiency, Cell Movement, Chemotaxis, Leukocyte, Corneal Injuries metabolism, Corneal Injuries pathology, Epithelium, Corneal physiology, Female, Hyperemia blood, Macrophages physiology, Male, Mice, Mice, Inbred C57BL, Microcirculation, Microscopy, Electron, Models, Animal, Phagocytosis, Regeneration physiology, Vasculitis blood, Venules pathology, Wound Healing physiology, Blood Platelets physiology, CD18 Antigens physiology, Cell Degranulation, Cornea blood supply, Erythrocytes physiology, Hyperemia physiopathology, Mast Cells physiology, Neutrophils physiology, Transendothelial and Transepithelial Migration physiology, Vasculitis immunology, Venules metabolism

Abstract

Platelet extravasation during inflammation is under-appreciated. In wild-type (WT) mice, a central corneal epithelial abrasion initiates neutrophil (PMN) and platelet extravasation from peripheral limbal venules. The same injury in mice expressing low levels of the β 2 -integrin, CD18 (CD18 hypo mice) shows reduced platelet extravasation with PMN extravasation apparently unaffected. To better define the role of CD18 on platelet extravasation, we focused on two relevant cell types expressing CD18: PMNs and mast cells. Following corneal abrasion in WT mice, we observed not only extravasated PMNs and platelets but also extravasated erythrocytes (RBCs). Ultrastructural observations of engorged limbal venules showed platelets and RBCs passing through endothelial pores. In contrast, injured CD18 hypo mice showed significantly less venule engorgement and markedly reduced platelet and RBC extravasation; mast cell degranulation was also reduced compared to WT mice. Corneal abrasion in mast cell-deficient (Kit W-sh/W-sh ) mice showed less venule engorgement, delayed PMN extravasation, reduced platelet and RBC extravasation and delayed wound healing compared to WT mice. Finally, antibody-induced depletion of circulating PMNs prior to corneal abrasion reduced mast cell degranulation, venule engorgement, and extravasation of PMNs, platelets, and RBCs. In summary, in the injured cornea, platelet and RBC extravasation depends on CD18, PMNs, and mast cell degranulation.

Published

2021

2. SNAP23 is essential for platelet and mast cell development and required in connective tissue mast cells for anaphylaxis.

Author

Cardenas RA, Gonzalez R, Sanchez E, Ramos MA, Cardenas EI, Rodarte AI, Alcazar-Felix RJ, Isaza A, Burns AR, Heidelberger R, and Adachi R

Subjects

Anaphylaxis genetics, Anaphylaxis pathology, Animals, Blood Platelets pathology, Connective Tissue pathology, Exocytosis genetics, Exocytosis immunology, Mast Cells pathology, Mice, Mice, Knockout, Qb-SNARE Proteins genetics, Qc-SNARE Proteins genetics, Secretory Vesicles genetics, Secretory Vesicles immunology, Anaphylaxis immunology, Blood Platelets immunology, Connective Tissue immunology, Mast Cells immunology, Qb-SNARE Proteins immunology, Qc-SNARE Proteins immunology

Abstract

Degranulation, a fundamental effector response from mast cells (MCs) and platelets, is an example of regulated exocytosis. This process is mediated by SNARE proteins and their regulators. We have previously shown that several of these proteins are essential for exocytosis in MCs and platelets. Here, we assessed the role of the SNARE protein SNAP23 using conditional knockout mice, in which SNAP23 was selectively deleted from either the megakaryocyte/platelet or connective tissue MC lineages. We found that removal of SNAP23 in platelets results in severe defects in degranulation of all three platelet secretory granule types, i.e., alpha, dense, and lysosomal granules. The mutation also induces thrombocytopenia, abnormal platelet morphology and activation, and reduction in the number of alpha granules. Therefore, the degranulation defect might not be secondary to an intrinsic failure of the machinery mediating regulated exocytosis in platelets. When we removed SNAP23 expression in MCs, there was a complete developmental failure in vitro and in vivo. The developmental defects in platelets and MCs and the abnormal translocation of membrane proteins to the surface of platelets indicate that SNAP23 is also involved in constitutive exocytosis in these cells. The MC conditional deletant animals lacked connective tissue MCs, but their mucosal MCs were normal and expanded in response to an antigenic stimulus. We used this mouse to show that connective tissue MCs are required and mucosal MCs are not sufficient for an anaphylactic response., Competing Interests: Conflict of interest The authors declare that they have no conflicts of interest with the contents of this article., (Copyright © 2021 The Authors. Published by Elsevier Inc. All rights reserved.)

Published

2021

3. Munc18-2, but not Munc18-1 or Munc18-3, regulates platelet exocytosis, hemostasis, and thrombosis.

Author

Cardenas EI, Gonzalez R, Breaux K, Da Q, Gutierrez BA, Ramos MA, Cardenas RA, Burns AR, Rumbaut RE, and Adachi R

Subjects

Animals, Blood Platelets pathology, Disease Models, Animal, Mice, Mice, Knockout, Munc18 Proteins genetics, Secretory Vesicles genetics, Secretory Vesicles pathology, Thrombosis genetics, Thrombosis pathology, Blood Platelets metabolism, Exocytosis, Hemostasis, Munc18 Proteins metabolism, Secretory Vesicles metabolism, Thrombosis metabolism

Abstract

Platelet degranulation, a form of regulated exocytosis, is crucial for hemostasis and thrombosis. Exocytosis in platelets is mediated by SNARE proteins, and in most mammalian cells this process is controlled by Munc18 (mammalian homolog of Caenorhabditis elegans uncoordinated gene 18) proteins. Platelets express all Munc18 paralogs (Munc18-1, -2, and -3), but their roles in platelet secretion and function have not been fully characterized. Using Munc18-1, -2, and -3 conditional knockout mice, here we deleted expression of these proteins in platelets and assessed granule exocytosis. We measured products secreted by each type of platelet granule and analyzed EM platelet profiles by design-based stereology. We observed that the removal of Munc18-2 ablates the release of alpha, dense, and lysosomal granules from platelets, but we found no exocytic role for Munc18-1 or -3 in platelets. In vitro , Munc18-2-deficient platelets exhibited defective aggregation at low doses of collagen and impaired thrombus formation under shear stress. In vivo , megakaryocyte-specific Munc18-2 conditional knockout mice had a severe hemostatic defect and prolonged arterial and venous bleeding times. They were also protected against arterial thrombosis in a chemically induced model of arterial injury. Taken together, our results indicate that Munc18-2, but not Munc18-1 or Munc18-3, is essential for regulated exocytosis in platelets and platelet participation in thrombosis and hemostasis.

Published

2019

4. Platelet Munc13-4 regulates hemostasis, thrombosis and airway inflammation.

Author

Cardenas EI, Breaux K, Da Q, Flores JR, Ramos MA, Tuvim MJ, Burns AR, Rumbaut RE, and Adachi R

Subjects

Animals, Biomarkers, Disease Models, Animal, Disease Susceptibility, Exocytosis, Hypersensitivity metabolism, Hypersensitivity pathology, Membrane Proteins metabolism, Mice, Mice, Knockout, Platelet Activation, Secretory Vesicles metabolism, Thrombosis blood, Blood Platelets metabolism, Hemostasis genetics, Hypersensitivity etiology, Membrane Proteins genetics, Thrombosis etiology

Abstract

Platelet degranulation is crucial for hemostasis and may participate in inflammation. Exocytosis in platelets is mediated by SNARE proteins and should be controlled by Munc13 proteins. We found that platelets express Munc13-2 and -4. We assessed platelet granule exocytosis in Munc13-2 and -4 global and conditional knockout (KO) mice, and observed that deletion of Munc13-4 ablates dense granule release and indirectly impairs alpha granule exocytosis. We found no exocytic role for Munc13-2 in platelets, not even in the absence of Munc13-4. In vitro , Munc13-4-deficient platelets exhibited defective aggregation at low doses of collagen. In a flow chamber assay, we observed that Munc13-4 acted as a rate-limiting factor in the formation of thrombi. In vivo , we observed a dose-dependency between Munc13-4 expression in platelets and both venous bleeding time and time to arterial thrombosis. Finally, in a model of allergic airway inflammation, we found that platelet-specific Munc13-4 KO mice had a reduction in airway hyper-responsiveness and eosinophilic inflammation. Taken together, our results indicate that Munc13-4-dependent platelet dense granule release plays essential roles in hemostasis, thrombosis and allergic inflammation., (Copyright© 2018 Ferrata Storti Foundation.)

Published

2018

5. Platelet recruitment promotes keratocyte repopulation following corneal epithelial abrasion in the mouse.

Author

Lam FW, Phillips J, Landry P, Magadi S, Smith CW, Rumbaut RE, and Burns AR

Subjects

Animals, Blood Platelets metabolism, Blood Platelets pathology, Corneal Injuries genetics, Corneal Keratocytes cytology, Epithelium, Corneal cytology, Epithelium, Corneal immunology, Epithelium, Corneal metabolism, Gene Deletion, Male, Mice, Inbred C57BL, P-Selectin genetics, P-Selectin immunology, Blood Platelets immunology, Corneal Injuries immunology, Corneal Injuries pathology, Corneal Keratocytes pathology, Epithelium, Corneal pathology, Wound Healing

Abstract

Corneal abrasion not only damages the epithelium but also induces stromal keratocyte death at the site of injury. While a coordinated cascade of inflammatory cell recruitment facilitates epithelial restoration, it is unclear if this cascade is necessary for keratocyte recovery. Since platelet and neutrophil (PMN) recruitment after corneal abrasion is beneficial to epithelial wound healing, we wanted to determine if these cells play a role in regulating keratocyte repopulation after epithelial abrasion. A 2 mm diameter central epithelial region was removed from the corneas of C57BL/6 wildtype (WT), P-selectin deficient (P-sel-/-), and CD18 hypomorphic (CD18hypo) mice using the Algerbrush II. Corneas were studied at 6h intervals out to 48h post-injury to evaluate platelet and PMN cell numbers; additional corneas were studied at 1, 4, 14, and 28 days post injury to evaluate keratocyte numbers. In WT mice, epithelial abrasion induced a loss of anterior central keratocytes and keratocyte recovery was rapid and incomplete, reaching ~70% of uninjured baseline values by 4 days post-injury but no further improvement at 28 days post-injury. Consistent with a beneficial role for platelets and PMNs in wound healing, keratocyte recovery was significantly depressed at 4 days post-injury (~30% of uninjured baseline) in P-sel-/- mice, which are known to have impaired platelet and PMN recruitment after corneal abrasion. Passive transfer of platelets from WT, but not P-sel-/-, into P-sel-/- mice prior to injury restored anterior central keratocyte numbers at 4 days post-injury to P-sel-/- uninjured baseline levels. While PMN infiltration in injured CD18hypo mice was similar to injured WT mice, platelet recruitment was markedly decreased and anterior central keratocyte recovery was significantly reduced (~50% of baseline) at 4-28 days post-injury. Collectively, the data suggest platelets and platelet P-selectin are critical for efficient keratocyte recovery after corneal epithelial abrasion.

Published

2015

6. Platelets enhance neutrophil transendothelial migration via P-selectin glycoprotein ligand-1.

Author

Lam FW, Burns AR, Smith CW, and Rumbaut RE

Subjects

Animals, Antibodies, Blocking pharmacology, Blood Cell Count, Cell Movement physiology, Cell Separation, Epithelium, Corneal physiology, Humans, Immunohistochemistry, In Vitro Techniques, Male, Membrane Glycoproteins antagonists & inhibitors, Membrane Glycoproteins genetics, Mice, Mice, Inbred C57BL, Mice, Knockout, P-Selectin genetics, Blood Platelets physiology, Endothelial Cells physiology, Endothelium, Vascular physiology, Membrane Glycoproteins physiology, Neutrophils physiology, P-Selectin physiology

Abstract

Platelets are increasingly recognized as important for inflammation in addition to thrombosis. Platelets promote the adhesion of neutrophils [polymorphonuclear neutrophils (PMNs)] to the endothelium; P-selectin and P-selectin glycoprotein ligand (PSGL)-1 have been suggested to participate in these interactions. Whether platelets also promote PMN transmigration across the endothelium is less clear. We tested the hypothesis that platelets enhance PMN transmigration across the inflamed endothelium and that PSGL-1 is involved. We studied the effects of platelets on PMN transmigration in vivo and in vitro using a well-characterized corneal injury model in C57BL/6 mice and IL-1β-stimulated human umbilical vein endothelial cells (HUVECs) under static and dynamic conditions. In vivo, platelet depletion altered PMN emigration from limbal microvessels after injury, with decreased emigration 6 and 12 h after injury. Both PSGL-1-/- and P-selectin-/- mice, but not Mac-1-/- mice, also had reduced PMN emigration at 12 h after injury relative to wild-type control mice. In the in vitro HUVEC model, platelets enhanced PMN transendothelial migration under static and dynamic conditions independent of firm adhesion. Anti-PSGL-1 antibodies markedly inhibited platelet-PMN aggregates, as assessed by flow cytometry, and attenuated the effect of platelets on PMN transmigration under static conditions without affecting firm adhesion. These data support the notion that platelets enhance neutrophil transmigration across the inflamed endothelium both in vivo and in vitro, via a PSGL-1-dependent mechanism.

Published

2011

7. gamma delta T cells are necessary for platelet and neutrophil accumulation in limbal vessels and efficient epithelial repair after corneal abrasion.

Author

Li Z, Burns AR, Rumbaut RE, and Smith CW

Subjects

Animals, CD11a Antigen genetics, CD11a Antigen metabolism, Cell Movement, Cornea metabolism, Epithelial Cells cytology, Epithelium metabolism, Epithelium pathology, Intercellular Adhesion Molecule-1 genetics, Intercellular Adhesion Molecule-1 metabolism, Leukocytes cytology, Leukocytes physiology, Lymphocyte Function-Associated Antigen-1 genetics, Lymphocyte Function-Associated Antigen-1 metabolism, Mice, Mice, Inbred C57BL, Mice, Knockout, P-Selectin genetics, P-Selectin metabolism, Receptors, Antigen, T-Cell, gamma-delta genetics, Receptors, Antigen, T-Cell, gamma-delta metabolism, T-Lymphocytes cytology, Wound Healing, Blood Platelets metabolism, Cornea blood supply, Corneal Injuries, Epithelial Cells physiology, Neutrophils metabolism, T-Lymphocyte Subsets, T-Lymphocytes metabolism

Abstract

Corneal epithelial abrasion in C57BL/6 mice induces an inflammatory response with peak accumulation of neutrophils in the corneal stroma within 12 hours. Platelets localize in the limbal vessels throughout the same time course as neutrophils and contribute to wound healing because antibody-dependent depletion of platelets retards epithelial division and wound closure. In the present study, T cells in the limbal epithelium were found to predominantly express the gammadelta T-cell receptor (TCR). Corneal abrasion in wild-type, CD11a(-/-), and P-sel(-/-) mice increased the numbers of gammadelta T cells in the limbal and peripheral corneal epithelium and in the corneal stroma adjacent to the limbal blood vessels. Intercellular adhesion molecule (ICAM)-1(-/-) mice exhibited a reduction in gammadelta T-cell accumulation. TCRdelta(-/-) mice exhibited reduced inflammation and delayed epithelial wound healing as evidenced by delayed wound closure, reduced epithelial cell division, reduced neutrophil infiltration, and reduced epithelial cell density at 96 hours after wounding. TCRdelta(-/-) mice also exhibited >60% reduction in platelet localization in the limbus despite similar platelet counts and platelet function assessed with an in vivo thrombosis model. These results are consistent with the conclusion that gammadelta T cells are necessary for efficient inflammation, platelet localization in the limbus, and epithelial wound healing after corneal abrasion.

Published

2007

8. Platelet response to corneal abrasion is necessary for acute inflammation and efficient re-epithelialization.

Author

Li Z, Rumbaut RE, Burns AR, and Smith CW

Subjects

Animals, Cell Movement, Cornea metabolism, Cornea ultrastructure, Fluorescent Antibody Technique, Indirect, Mice, Mice, Inbred C57BL, Mice, Knockout, Neutrophils physiology, P-Selectin physiology, Thrombocytopenia metabolism, Blood Platelets physiology, Corneal Injuries, Epithelium, Corneal physiology, Keratitis metabolism, Wound Healing physiology

Abstract

Purpose: Adhesion molecules play a critical role in leukocyte emigration to wound sites, but differences are evident in different vascular beds. In this study, the contributions of P-selectin to neutrophil emigration into the cornea after central epithelial abrasion were investigated., Methods: Re-epithelialization, neutrophil influx, and platelet accumulation were assessed in C57BL/6 mice after removal of a 2-mm diameter area of central corneal epithelium that did not directly injure the limbal vessels or the avascular stroma of the cornea. Comparisons were made between wild-type (WT) mice and mice with targeted deletions of genes for P-selectin, CD18, or CD54, or mice with antibody-induced neutropenia or thrombocytopenia., Results: After central corneal epithelial abrasion, platelets localized in the limbal vessels and neutrophils emigrated from the limbal vessels to the region of the epithelial wound. There was temporal correspondence of platelet and neutrophil localization, peaking within 12 hours of wounding. Platelet accumulation, neutrophil emigration and corneal epithelial healing as measured by wound closure, basal epithelial cell density, and epithelial cell division were significantly reduced in P-selectin-deficient mice (P-sel(-/-)). Anti-GP1balpha antibody-induced thrombocytopenia in WT mice significantly reduced platelet and neutrophil accumulation and wound healing. Passive transfer of wild-type platelets into P-sel(-/-) mice significantly restored platelet localization in limbal vessels, neutrophil emigration, epithelial cell division, and epithelial cell migration into the abraded region of the cornea., Conclusions: Platelet localization in the limbus of abraded corneas contributes to re-epithelialization, and P-selectin provides a necessary step in this process.

Published

2006

9. Microvascular thrombosis models in venules and arterioles in vivo.

Author

Rumbaut RE, Slaff DW, and Burns AR

Subjects

Animals, Models, Animal, Arterioles physiology, Blood Platelets physiology, Thrombosis physiopathology, Venules physiology

Abstract

Platelets are intimately involved in hemostasis and thrombosis. Under physiological conditions, circulating platelets do not interact with microvascular walls. However, in response to microvascular injury, platelet adhesion and subsequent thrombus formation may be observed in venules and arterioles in vivo. Numerous intravital video microscopy techniques have been described to induce and monitor the formation of microvascular thrombi. The mechanisms of microvascular injury vary widely among different models. Some models induce platelet activation with minimal effects on endothelium, others induce endothelial inflammation or injury, while other models lead to thrombus formation associated with endothelial denudation. The molecular mechanisms mediating platelet-vessel wall adhesive interactions differ among various models. In some instances, differences in responses between venules and arterioles are described that cannot be explained solely by hemodynamic factors. Several models for induction of microvascular thrombosis in vivo are outlined in this review, with a focus on the mechanisms of injury and thrombus formation, as well as on differences in responses between venules and arterioles. Recognizing these characteristics should help investigators select an appropriate model for studying microvascular thrombosis in vivo.

Published

2005

10. Venous levels of shear support neutrophil-platelet adhesion and neutrophil aggregation in blood via P-selectin and beta2-integrin.

Author

Konstantopoulos K, Neelamegham S, Burns AR, Hentzen E, Kansas GS, Snapp KR, Berg EL, Hellums JD, Smith CW, McIntire LV, and Simon SI

Subjects

Abciximab, Adult, Antibodies, Monoclonal, Blood Platelets chemistry, Blood Platelets ultrastructure, Cations metabolism, Cell Adhesion drug effects, Cell Adhesion physiology, Cell Aggregation drug effects, Cell Aggregation physiology, Chelating Agents pharmacology, Edetic Acid pharmacology, Female, Flow Cytometry, Humans, Iloprost pharmacology, Immunoglobulin Fab Fragments, Kinetics, Macrophage-1 Antigen metabolism, Male, Microscopy, Electron, Middle Aged, Neutrophils chemistry, Neutrophils ultrastructure, Platelet Aggregation Inhibitors pharmacology, Platelet Glycoprotein GPIIb-IIIa Complex immunology, Stress, Mechanical, Veins, Blood Platelets cytology, CD18 Antigens metabolism, Neutrophils cytology, P-Selectin metabolism

Abstract

Background: After activation, platelets adhere to neutrophils via P-selectin and beta2-integrin. The molecular mechanisms and adhesion events in whole blood exposed to venous levels of hydrodynamic shear in the absence of exogenous activation remain unknown., Methods and Results: Whole blood was sheared at approximately 100 s(-1). The kinetics of neutrophil-platelet adhesion and neutrophil aggregation were measured in real time by flow cytometry. P-selectin was upregulated to the platelet surface in response to shear and was the primary factor mediating neutrophil-platelet adhesion. The extent of neutrophil aggregation increased linearly with platelet adhesion to neutrophils. Blocking either P-selectin, its glycoprotein ligand PSGL-1, or both simultaneously by preincubation with a monoclonal antibody resulted in equivalent inhibition of neutrophil-platelet adhesion (approximately 30%) and neutrophil aggregation (approximately 70%). The residual amount of neutrophil adhesion was blocked with anti-CD11b/CD18. Treatment of blood with prostacyclin analogue ZK36374, which raises cAMP levels in platelets, blocked P-selectin upregulation and neutrophil aggregation to baseline. Complete abrogation of platelet-neutrophil adhesion required both ZK36374 and anti-CD18. Electron microscopic observations of fixed blood specimens revealed that platelets augmented neutrophil aggregation both by forming bridges between neutrophils and through contact-mediated activation., Conclusions: The results are consistent with a model in which venous levels of shear support platelet adherence to neutrophils via P-selectin binding PSGL-1. This interaction alone is sufficient to mediate neutrophil aggregation. Abrogation of platelet adhesion and aggregation requires blocking Mac-1 in addition to PSGL-1 or P-selectin. The described mechanisms are likely of key importance in the pathogenesis and progression of thrombotic disorders that are exacerbated by leukocyte-platelet aggregation.

Published

1998