Your search keyword '"Lee, Winston Y."' showing total 5 results

1. Neutrophil migration across intestinal epithelium: evidence for a role of CD44 in regulating detachment of migrating cells from the luminal surface.

Author

Brazil JC, Lee WY, Kolegraff KN, Nusrat A, Parkos CA, and Louis NA

Subjects

Antigenic Variation physiology, Caco-2 Cells, Cell Adhesion immunology, Cells, Cultured, Endothelium, Vascular cytology, Endothelium, Vascular immunology, Endothelium, Vascular metabolism, HT29 Cells, HeLa Cells, Humans, Inflammation Mediators physiology, Intestinal Mucosa cytology, Neutrophils cytology, Protein Isoforms physiology, Surface Properties, Cell Movement immunology, Hyaluronan Receptors physiology, Intestinal Mucosa immunology, Intestinal Mucosa metabolism, Neutrophils immunology, Neutrophils metabolism

Abstract

The migration of polymorphonuclear leukocytes (PMNs) across the intestinal epithelium is a histopathological hallmark of many mucosal inflammatory diseases including inflammatory bowel disease. The terminal transmigration step is the detachment of PMNs from the apical surface of the epithelium and their subsequent release into the intestinal lumen. The current study sought to identify epithelial proteins involved in the regulation of PMN migration across intestinal epithelium at the stage at which PMNs reach the apical epithelial surface. A panel of Abs reactive with IFN-γ-stimulated T84 intestinal epithelial cells was generated. Screening efforts identified one mAb, GM35, that prevented PMN detachment from the apical epithelial surface. Microsequencing studies identified the GM35 Ag as human CD44. Transfection studies confirmed this result by demonstrating the loss of the functional activity of the GM35 mAb following attenuation of epithelial CD44 protein expression. Immunoblotting and immunofluorescence revealed the GM35 Ag to be an apically expressed v6 variant exon-containing form of human CD44 (CD44v6). ELISA analysis demonstrated the release of soluble CD44v6 by T84 cells during PMN transepithelial migration. In addition, the observed release of CD44v6 was blocked by GM35 treatment, supporting a connection between CD44v6 release and PMN detachment. Increased expression of CD44v6 and the GM35 Ag was detected in inflamed ulcerative colitis tissue. This study demonstrates that epithelial-expressed CD44v6 plays a role in PMN clearance during inflammatory episodes through regulation of the terminal detachment of PMNs from the apical epithelial surface into the lumen of the intestine.

Published

2010

2. CD47 and TLR-2 cross-talk regulates neutrophil transmigration.

Author

Chin AC, Fournier B, Peatman EJ, Reaves TA, Lee WY, and Parkos CA

Subjects

Animals, Bacterial Proteins physiology, Cell Migration Inhibition immunology, Chemotaxis, Leukocyte immunology, Humans, Lipopeptides physiology, Mice, Mice, Inbred C57BL, Mice, Knockout, Neutrophil Infiltration genetics, Neutrophils microbiology, Neutrophils pathology, Signal Transduction immunology, Toll-Like Receptor 2 deficiency, Toll-Like Receptor 2 genetics, CD47 Antigen physiology, Neutrophil Infiltration immunology, Neutrophils immunology, Receptor Cross-Talk immunology, Toll-Like Receptor 2 physiology, Toll-Like Receptor 6 physiology

Abstract

Neutrophil (PMN) infiltration into tissues is a hallmark of acute inflammation and is crucial for the rapid removal of microbial pathogens. Previous studies have shown that PMN transmigration is regulated by the cell surface protein CD47. However this phenomenon in the context of microbial invasion and subsequent TLR signaling is poorly understood. In this study, we assessed the role of TLR2 and CD47 costimulation in regulating PMN transmigration. Human PMN transmigration across acellular collagen-coated filters toward the bacterial chemoattractant fMLP was more significantly inhibited by MALP-2 (TLR2/6 agonist) than Pam(3)CSK(4) (TLR2/1 agonist). Subsequent experiments demonstrated that treatment with MALP-2 or anti-human CD47 mAbs delayed human PMN transfilter migration, while combined treatment led to further delayed inhibition. Interestingly, stimulation of PMNs with MALP-2 resulted in an increase in surface expression of CD11b, but not CD47. In experiments addressing the role of TLR agonists in regulating CD47-mediated PMN transmigration, incubation with MALP-2 or with anti-mouse CD47 mAbs did not inhibit transfilter migration of TLR2(-/-) or MyD88(-/-)-deficient murine bone marrow-derived PMNs. Similarly, inhibition of MyD88 homodimerization reversed the attenuation of human PMN transmigration induced by MALP-2 or anti-human CD47 mAbs. Separate experiments demonstrated that CD47(-/-) murine bone marrow-derived PMNs exhibited 4-fold decreased sensitivity toward MALP-2. Collectively, these findings suggest that activation of CD47 signaling enhances PMN sensitivity toward TLR2 activation which, in turn, signals their arrival at a site of invasion and may facilitate antimicrobial function.

Published

2009

3. Neutrophil-mediated activation of epithelial protease-activated receptors-1 and -2 regulates barrier function and transepithelial migration.

Author

Chin AC, Lee WY, Nusrat A, Vergnolle N, and Parkos CA

Subjects

Cathepsin G, Cathepsins pharmacology, Cell Movement drug effects, Cells, Cultured, Chemotactic Factors immunology, Chemotactic Factors metabolism, Coculture Techniques, Gene Expression Regulation drug effects, Gene Expression Regulation immunology, Humans, Inflammatory Bowel Diseases metabolism, Inflammatory Bowel Diseases pathology, Intestinal Mucosa metabolism, Intestinal Mucosa pathology, Myeloblastin pharmacology, Neutrophil Infiltration drug effects, Neutrophils metabolism, Neutrophils pathology, Pancreatic Elastase pharmacology, Permeability drug effects, Receptor, PAR-1 antagonists & inhibitors, Receptor, PAR-1 metabolism, Receptor, PAR-2 antagonists & inhibitors, Receptor, PAR-2 metabolism, Serine Endopeptidases pharmacology, Signal Transduction drug effects, Signal Transduction immunology, Substrate Specificity, Tight Junctions immunology, Cell Movement immunology, Inflammatory Bowel Diseases immunology, Intestinal Mucosa immunology, Neutrophil Infiltration immunology, Neutrophils immunology, Receptor, PAR-1 immunology, Receptor, PAR-2 immunology

Abstract

Neutrophil (PMN) infiltration and associated release of serine proteases contribute to epithelial injury during active phases of mucosal disorders such as inflammatory bowel disease. Previous studies have demonstrated that PMN contact with basolateral surfaces of intestinal epithelial cells in the presence of a chemoattractant results in disruption of barrier function even without transmigration. Similarly, serine protease-mediated activation of epithelial protease-activated receptors (PARs) has been shown to increase permeability. In this study, we assessed whether transmigrating PMNs can regulate barrier function through epithelial PAR activation. Transepithelial resistance (TER) decreased significantly after PMN contact with basolateral surfaces of T84 monolayers or after incubation with PMN elastase and proteinase-3, but not cathepsin G. Inhibition of PMN serine proteases, but not selective inhibition of elastase or cathepsin G, prevented the fall in TER induced by PMN contact and blocked PMN transepithelial migration. Basolateral, but not apical, PAR-1 and -2 activation with selective agonists also decreased TER. PAR-1 and -2 were localized intracellularly and in close proximity to lateral surfaces beneath tight junctions, and expression was increased in colonic mucosa from individuals with Crohn's disease. Combined, but not individual, transfection with small interfering RNAs targeted against epithelial PAR-1 and -2, prevented the fall in TER induced by PMN contact. Furthermore, basolateral PAR-1 and -2 activation induced phosphorylation of myosin L chain kinase and regulatory myosin L chain. Lastly, epithelial PAR-1 and -2 knockdown decreased the rate of PMN transepithelial migration. These results suggest that protease-mediated epithelial PAR-1 and -2 activation, by migrating PMNs, induces signaling events that increase epithelial permeability thereby facilitates PMN transepithelial migration.

Published

2008

4. Annexin A1 regulates intestinal mucosal injury, inflammation, and repair.

Author

Babbin BA, Laukoetter MG, Nava P, Koch S, Lee WY, Capaldo CT, Peatman E, Severson EA, Flower RJ, Perretti M, Parkos CA, and Nusrat A

Subjects

Animals, Annexin A1 biosynthesis, Annexin A1 deficiency, Annexin A1 genetics, Colitis chemically induced, Colitis metabolism, Colitis pathology, Dextran Sulfate toxicity, Female, Genetic Predisposition to Disease, Inflammation Mediators metabolism, Intestinal Mucosa drug effects, Mice, Mice, Inbred BALB C, Mice, Knockout, Severity of Illness Index, Wound Healing drug effects, Annexin A1 physiology, Inflammation Mediators physiology, Intestinal Mucosa metabolism, Intestinal Mucosa pathology, Wound Healing immunology

Abstract

During mucosal inflammation, a complex array of proinflammatory and protective mechanisms regulates inflammation and severity of injury. Secretion of anti-inflammatory mediators is a mechanism that is critical in controlling inflammatory responses and promoting epithelial restitution and barrier recovery. AnxA1 is a potent anti-inflammatory protein that has been implicated to play a critical immune regulatory role in models of inflammation. Although AnxA1 has been shown to be secreted in intestinal mucosal tissues during inflammation, its potential role in modulating the injury/inflammatory response is not understood. In this study, we demonstrate that AnxA1-deficient animals exhibit increased susceptibility to dextran sulfate sodium (DSS)-induced colitis with greater clinical morbidity and histopathologic mucosal injury. Furthermore, impaired recovery following withdrawal of DSS administration was observed in AnxA1 (-/-) animals compared with wild-type (WT) control mice that was independent of inflammatory cell infiltration. Since AnxA1 exerts its anti-inflammatory properties through stimulation of ALX/FPRL-1, we explored the role of this receptor-ligand interaction in regulating DSS-induced colitis. Interestingly, treatment with an ALX/FPRL-1 agonist, 15-epi-lipoxin A4 reversed the enhanced sensitivity of AnxA1 (-/-) mice to DSS colitis. In contrast, 15-epi-lipoxin A4 did not significantly improve the severity of disease in WT animals. Additionally, differential expression of ALX/FPLR-1 in control and DSS-treated WT and AnxA1-deficient animals suggested a potential role for AnxA1 in regulating ALX/FPRL-1 expression under pathophysiological conditions. Together, these results support a role of endogenous AnxA1 in the protective and reparative properties of the intestinal mucosal epithelium.

Published

2008

5. Novel structural determinants on SIRP alpha that mediate binding to CD47.

Author

Lee WY, Weber DA, Laur O, Severson EA, McCall I, Jen RP, Chin AC, Wu T, Gernert KM, and Parkos CA

Subjects

Animals, Antibodies, Monoclonal immunology, Antigen-Antibody Reactions, Antigens, Differentiation chemistry, COS Cells, Cell Membrane immunology, Chlorocebus aethiops, Humans, Immunoglobulin G immunology, Models, Molecular, Molecular Sequence Data, Protein Binding, Protein Structure, Tertiary, Receptors, Cell Surface chemistry, Receptors, Cell Surface immunology, Receptors, Immunologic chemistry, Recombinant Proteins chemistry, Recombinant Proteins immunology, Antigens, Differentiation immunology, CD47 Antigen immunology, Receptors, Immunologic immunology

Abstract

Signal regulatory proteins (SIRP-alpha, -beta, and -gamma) are important regulators of several innate immune functions that include leukocyte migration. Membrane distal (D1) domains of SIRPalpha and SIRPgamma, but not SIRPbeta, mediate binding to a cellular ligand termed CD47. Because the extracellular domains of all SIRPs are highly homologous, we hypothesized that some of the 16 residues unique to SIRPalpha.D1 mediate binding to CD47. By site-directed mutagenesis, we determined that SIRPalpha binding to CD47 is independent of N-glycosylation. We also identified three residues critical for CD47 binding by exchanging residues on SIRPalpha with corresponding residues from SIRPbeta. Cumulative substitutions of the critical residues into SIRPbeta resulted in de novo binding of the mutant protein to CD47. Homology modeling of SIRPalpha.D1 revealed topological relationships among critical residues and allowed the identification of critical residues common to SIRPalpha and SIRPbeta. Mapping these critical residues onto the recently reported crystal structure of SIRPalpha.D1 revealed a novel region that is required for CD47 binding and is distinct and lateral to another putative CD47 binding site described on that crystal structure. The importance of this lateral region in mediating SIRPalpha.D1 binding to CD47 was confirmed by epitope mapping analyses of anti-SIRP Abs. These observations highlight a complex nature of the ligand binding requirements for SIRPalpha that appear to be dependent on two distinct but adjacent regions on the membrane distal Ig loop. A better understanding of the structural basis of SIRPalpha/CD47 interactions may provide insights into therapeutics targeting pathologic inflammation.

Published

2007