Abstract

Leukocyte adhesion to endothelial cells (EC) is a central process in the pathogenesis of inflammatory disease. Specialized receptors for initial attachment enable blood-borne cells to initiate slow rolling venules. Subsequently, activating stimuli trigger engagement of activation- dependent integrins which, in turn, mediate firm attachment. This project is aimed at defining the role of transmembrane and intracellular (TM/IC) segments of leukocyte adhesion molecules in the early steps of this cascade. Using immunoelectron microscopy, it was found that many adhesion molecules display a distinct surface topography. L-selectin (CD62L), a specialized receptor for contact initiation, is clustered on microvilli. In contrast, CD44, an adhesion molecule with undefined intravascular function, is restricted to the planar cell body. Based on preliminary findings, it is proposed that the conspicuous topographies of L-selectin and CD44 are differentially regulated by their TM/IC domains and that topography itself is an important determinant of adhesion under flow. Microvillous receptors preferentially initiate attachment, whereas exclusion from microvilli limits a molecule's availability to situations when the cell has already been tethered. Following binding, TM/IC domains of L-selectin and CD44 may trigger differential activation pathways to signal ligation of ectodomains to the leukocyte. To investigate this concept, a panel of nine L1-2 lymphoma cell lines has been stably transfected with microvillous L-selectin, cell body CD44, E- selectin, and CD31 (both randomly distributed), and with chimeric genes encoding the TM/IC domains of one receptor and the ectodomain of another (aim 1). Transfectants will be used to study the importance of TM/IC domains in receptor topography using immunogold staining and scanning electron microscopy (aim 2). Topography-function relationships (aim 3) will be assessed in static and flow assays of cell binding to soluble and immobilized ligands. Cytochalasin-treated transfectants will also be used to study the general role of the cytoskeleton, and ezrin and moesin, two cytoskeletal proteins required for microvillous assembly, will be inhibited by antisense treatment and cytoplasmic loading with antibodies to determine the importance of microvilli in particular. Using intravital microscopy the in vivo relevance of topographic distribution for leukocyte trafficking in acute inflammation and in physiologic homing to high endothelial venules will be defined. Finally, the role of TM/IC domains in differential cytoplasmic Ca2 plus/minus mobilization by crosslinked receptors will be assessed, and additional mutant transfectants will be generated to identify distinct regions within TM/IC domains that are important for their function in topography and Ca2+ signaling (aim 4). Together, these studies will dissect the complex interplay of biophysical, molecular, biochemical, and cellular mechanisms that determine the earliest prerequisite steps in microvascular leukocyte adhesion.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Heart, Lung, and Blood Institute (NHLBI)
Type
Research Project (R01)
Project #
5R01HL054936-05
Application #
6184323
Study Section
Pathology A Study Section (PTHA)
Project Start
1996-05-01
Project End
2001-05-09
Budget Start
2000-06-21
Budget End
2001-05-09
Support Year
5
Fiscal Year
2000
Total Cost
$351,186
Indirect Cost

  Institution

Name
Immune Disease Institute, Inc.
Department
Type
DUNS #
115524410
City
Boston
State
MA
Country
United States
Zip Code
02115

  Publications

Scimone, M Lucila; Aifantis, Iannis; Apostolou, Irina et al. (2006) A multistep adhesion cascade for lymphoid progenitor cell homing to the thymus. Proc Natl Acad Sci U S A 103:7006-11
Mempel, Thorsten R; Pittet, Mikael J; Khazaie, Khashayarsha et al. (2006) Regulatory T cells reversibly suppress cytotoxic T cell function independent of effector differentiation. Immunity 25:129-41
Rodrigo Mora, J; Von Andrian, U H (2006) Specificity and plasticity of memory lymphocyte migration. Curr Top Microbiol Immunol 308:83-116
Mora, J Rodrigo; Iwata, Makoto; Eksteen, Bertus et al. (2006) Generation of gut-homing IgA-secreting B cells by intestinal dendritic cells. Science 314:1157-60
Mora, J Rodrigo; von Andrian, Ulrich H (2006) T-cell homing specificity and plasticity: new concepts and future challenges. Trends Immunol 27:235-43
Mora, J Rodrigo; Cheng, Guiying; Picarella, Dominic et al. (2005) Reciprocal and dynamic control of CD8 T cell homing by dendritic cells from skin- and gut-associated lymphoid tissues. J Exp Med 201:303-16
Mazo, Irina B; Honczarenko, Marek; Leung, Harry et al. (2005) Bone marrow is a major reservoir and site of recruitment for central memory CD8+ T cells. Immunity 22:259-70
Halin, Cornelia; Scimone, M Lucila; Bonasio, Roberto et al. (2005) The S1P-analog FTY720 differentially modulates T-cell homing via HEV: T-cell-expressed S1P1 amplifies integrin activation in peripheral lymph nodes but not in Peyer patches. Blood 106:1314-22
Uchimura, Kenji; Gauguet, Jean-Marc; Singer, Mark S et al. (2005) A major class of L-selectin ligands is eliminated in mice deficient in two sulfotransferases expressed in high endothelial venules. Nat Immunol 6:1105-13
Cavanagh, Lois L; Bonasio, Roberto; Mazo, Irina B et al. (2005) Activation of bone marrow-resident memory T cells by circulating, antigen-bearing dendritic cells. Nat Immunol 6:1029-37

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