P-selectin glycoprotein ligand-1–deficient mice have impaired leukocyte tethering to E-selectin under flow

Xia, Lijun; Sperandio, Markus; Yago, Tadayuki; McDaniel, J. Michael; Cummings, Richard D.; Pearson‐White, Sonia; Ley, Klaus; McEver, Rodger P.

doi:10.1172/jci0214151

Cited by 201 publications

(180 citation statements)

References 61 publications

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“…If it is found that P-selectin and E-selectin can utilize endoglycan as a ligand, as is strongly suspected from its parallels to PSGL-1, the range of potential in vivo functions for this molecule would be further broadened since these selectins are found on platelets and/or activated vascular endothelium. Gene targeting approaches (52,53) and antibody blockade studies (49) have been essential in establishing the importance of PSGL-1 as a selectin ligand. Similar approaches will be necessary to gain a further understanding of endoglycan.…”

Section: Discussionmentioning

confidence: 99%

Endoglycan, a Member of the CD34 Family, Functions as an L-selectin Ligand through Modification with Tyrosine Sulfation and Sialyl Lewis x

Fieger

Sassetti²,

Rosen

2003

Journal of Biological Chemistry

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During lymphocyte homing to secondary lymphoid organs and instances of inflammatory trafficking, the rolling of leukocytes on vascular endothelium is mediated by transient interactions between L-selectin on leukocytes and several carbohydrate-modified ligands on the endothelium. Most L-selectin ligands such as CD34 and podocalyxin present sulfated carbohydrate structures (6-sulfated sialyl Lewis x or 6-sulfo-sLex) as a recognition determinant within their heavily glycosylated mucin domains. We recently identified endoglycan as a new member of the CD34 family. We report here that endoglycan, like the two other members of this family (CD34 and podocalyxin) can function as a L-selectin ligand. However, endoglycan employs a different binding mechanism, interacting with L-selectin through sulfation on two tyrosine residues and O-linked sLex structures that are presented within its highly acidic aminoterminal region. Our analysis establishes striking parallels with PSGL-1, a leukocyte ligand that interacts with all three selectins, mediating leukocyte-endothelial, leukocyte-leukocyte, and platelet-leukocyte interactions. Since the distribution of endoglycan includes hematopoietic precursors and leukocyte subpopulations, in addition to endothelial cells, our findings suggest several potential settings for endoglycan-mediated adhesion events.

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Section: Discussionmentioning

confidence: 99%

Endoglycan, a Member of the CD34 Family, Functions as an L-selectin Ligand through Modification with Tyrosine Sulfation and Sialyl Lewis x

Fieger

Sassetti²,

Rosen

2003

Journal of Biological Chemistry

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“…10 Antibody blockade of the N-terminal region of PSGL-1 inhibits rolling of leukocytes on P-selectin and L-selectin in vivo. 12,13 Elimination of PSGL-1 by gene targeting and homologous recombination reduces the number of neutrophils interacting with the endothelium, 14,15 alters the rolling velocity on P-selectin and on E-selectin, 14,16 and diminishes neutrophil recruitment into inflamed tissue. 15 In addition to its adhesive function, PSGL-1 is also known to initiate intracellular signaling events upon ligand engagement.…”

Section: Psgl-1mentioning

confidence: 99%

Mechanisms and Consequences of Neutrophil Interaction with the Endothelium

Zarbock

Ley

2008

The American Journal of Pathology

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Leukocyte recruitment into inflamed tissue proceeds in a cascade-like fashion. The first contact of neutrophils with the endothelium is mediated by selectins and their counterreceptors, followed by rolling of neutrophils along the endothelial wall of postcapillary venules and integrin-mediated arrest. While rolling, neutrophils collect different inflammatory signals that can activate several pathways. In addition to activation of neutrophils by ligation of G-protein-coupled receptors with chemokines and other chemoattractants, integrins and selectin ligands are also able to signal into the cell, where they initiate neutrophil extravasation, promote cytoskeletal rearrangement, and ultimately induce superoxide production and degranulation. These signaling pathways may be targeted by therapeutic interventions to inhibit specific functions of neutrophils without affecting others. This Review is focused on the signaling events during the interaction of neutrophils with the endothelium.

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“…The leukocyte mucin P-selectin glycoprotein ligand-1 (PSGL-1) is the dominant ligand for P-and L-selectin and an important ligand for E-selectin. 3,4 The manner in which selectins or their ligands distribute on cell surfaces has major influence on rolling behavior. 5 For example, L-selectin and PSGL-1 are located on tips of microvilli, 6,7 which enhances the initial tethering of leukocytes.…”

Section: Introductionmentioning

confidence: 99%

Clustering endothelial E-selectin in clathrin-coated pits and lipid rafts enhances leukocyte adhesion under flow

Setiadi

McEver

2008

Blood

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During inflammation, E-selectin expressed on cytokine-activated endothelial cells mediates leukocyte rolling under flow. E-selectin undergoes endocytosis and may associate with lipid rafts. We asked whether distribution of E-selectin in membrane domains affects its functions. E-selectin was internalized in transfected CHO cells or cytokine-activated human umbilical vein endothelial cells (HUVECs). Confocal microscopy demonstrated colocalization of E-selectin with ␣-adaptin, a clathrin-associated protein.Deleting the cytoplasmic domain of Eselectin or disrupting clathrin-coated pits with hypertonic medium blocked internalization of E-selectin, reduced colocalization of E-selectin with ␣-adaptin, and inhibited E-selectin-mediated neutrophil rolling under flow. Unlike CHO cells, HUVECs expressed a small percentage of E-selectin in lipid rafts. Even fewer neutrophils rolled on E-selectin in HUVECs treated with hypertonic medium and with methyl-␤-cyclodextrin, which disrupts lipid rafts. These data demonstrate that E-selectin clusters in both clathrin-coated pits and lipid rafts of endothelial cells but is internalized in clathrin-coated pits. Distribution in both domains markedly enhances E-selectin's ability to mediate leukocyte rolling under flow. IntroductionRecruitment of leukocytes into secondary lymphoid organs or inflamed tissues requires that the cells first tether to and roll on vascular surfaces. Interactions of selectins with their glycoconjugate ligands mediate tethering and rolling, 1 which precedes integrindependent deceleration, arrest, and transmigration of leukocytes across the endothelial cell layer. 2 L-selectin, expressed on leukocytes, binds to ligands on other leukocytes and on endothelial cells in lymph nodes and in some regions of inflammation. P-and E-selectin, expressed on activated platelets or endothelial cells, bind to ligands on leukocytes. The leukocyte mucin P-selectin glycoprotein ligand-1 (PSGL-1) is the dominant ligand for P-and L-selectin and an important ligand for E-selectin. 3,4 The manner in which selectins or their ligands distribute on cell surfaces has major influence on rolling behavior. 5 For example, L-selectin and PSGL-1 are located on tips of microvilli, 6,7 which enhances the initial tethering of leukocytes. 8 The extended length of P-selectin helps capture flowing neutrophils and slow their rolling velocities, presumably by increasing encounters with PSGL-1. 9 The dimeric structures of P-selectin and PSGL-1 allow them to form dimeric bonds that prolong tether duration and strength. 10 Membrane anchorage of L-selectin and P-selectin through binding of their cytoplasmic domains to cytosolic proteins favors rolling. L-selectin anchors through interactions of its cytoplasmic domain with the cytoskeleton to effectively engage its ligands under flow. 11 P-selectin uses a different mechanism to cluster on the cell surface. Thrombin or histamine mobilizes P-selectin from the membranes of Weibel-Palade bodies to the plasma membranes of endothelial cells. 12,13 Sequences in t...

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P-selectin glycoprotein ligand-1–deficient mice have impaired leukocyte tethering to E-selectin under flow

Cited by 201 publications

References 61 publications

Endoglycan, a Member of the CD34 Family, Functions as an L-selectin Ligand through Modification with Tyrosine Sulfation and Sialyl Lewis x

Endoglycan, a Member of the CD34 Family, Functions as an L-selectin Ligand through Modification with Tyrosine Sulfation and Sialyl Lewis x

Mechanisms and Consequences of Neutrophil Interaction with the Endothelium

Clustering endothelial E-selectin in clathrin-coated pits and lipid rafts enhances leukocyte adhesion under flow

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