Abstract

Cell death is a critical regulatory process in development, in homeostasis, and in disease. Many cell death triggers have been identified, although little is known about many of the molecular pathways that lead to cell death. Galectin-1, a member of a family of evolutionarily ancient lectins, induces death of thymocytes and T-cells. In mammals, galectin-1 is expressed in lymphoid tissues, at sites of inflammation, and in some types of cancer. Galectin-1 has also been shown to be immunosuppressive in several animal models of autoimmune disease. Galectin-1 induces cell death of transformed epithelial cells as well, so that galectin-1 mediated cell death may be a fundamental mechanism that regulates cell survival in many tissues. Other galectin family members have pro- or anti-apoptotic activities in different tissues, suggesting that different galectins may cooperate to regulate cell death. The goal of this application is to characterize the molecular mechanism of galectin-1 cell death, to understand the interaction of galectin-1 with glycoprotein receptors on the cell surface, and the downstream events that regulate cell death.
The Specific Aims are: 1. To define features of the T-cell surface receptors for galectin-l required to transmit the death signal. CD7 and CD43 are glycoprotein receptors for galectin-1. Features of the glycans and the polypeptides that are essential for sending the death signal will be identified. 2. To examine how galectin-l binding to T-cells results in molecular interactions to deliver the death signal. Galectin-1 binding results in a unique pattern of receptor reorganization on the T-cell surface. We will identify features of the receptors required for this interaction, and investigate whether receptor reorganization is required for cell death. Effects of galectin-1 on cytoskeletal linker proteins and on the actin cytoskeleton will be characterized. To examine cell-cell interactions that govern T-cell death, receptor reorganization during galectin-1 mediated binding of T-cells to thymic stromal cells will be examined. 3. To characterize intracellular components that regulate the galectin-l cell death pathway. We will examine the roles of the protein kinase C and protein phosphatase families of enzymes in regulating galectin1 cell death. We determine how galectin-3 expression regulates T-cell susceptibility to galectin-1.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of General Medical Sciences (NIGMS)
Type
Research Project (R01)
Project #
5R01GM063281-06
Application #
6636669
Study Section
Immunobiology Study Section (IMB)
Program Officer
Marino, Pamela
Project Start
1997-09-01
Project End
2005-05-31
Budget Start
2003-06-01
Budget End
2004-05-31
Support Year
6
Fiscal Year
2003
Total Cost
$258,638
Indirect Cost

  Institution

Name
University of California Los Angeles
Department
Pathology
Type
Schools of Medicine
DUNS #
092530369
City
Los Angeles
State
CA
Country
United States
Zip Code
90095

  Publications

Earl, Lesley A; Bi, Shuguang; Baum, Linda G (2011) Galectin multimerization and lattice formation are regulated by linker region structure. Glycobiology 21:6-12
Earl, Lesley A; Bi, Shuguang; Baum, Linda G (2010) N- and O-glycans modulate galectin-1 binding, CD45 signaling, and T cell death. J Biol Chem 285:2232-44
Nesmelova, Irina V; Ermakova, Elena; Daragan, Vladimir A et al. (2010) Lactose binding to galectin-1 modulates structural dynamics, increases conformational entropy, and occurs with apparent negative cooperativity. J Mol Biol 397:1209-30
Pang, Mabel; He, Jiale; Johnson, Pauline et al. (2009) CD45-mediated fodrin cleavage during galectin-1 T cell death promotes phagocytic clearance of dying cells. J Immunol 182:7001-8
Bi, Shuguang; Baum, Linda G (2009) Sialic acids in T cell development and function. Biochim Biophys Acta 1790:1599-610
Liu, Scot D; Whiting, Chan C; Tomassian, Tamar et al. (2008) Endogenous galectin-1 enforces class I-restricted TCR functional fate decisions in thymocytes. Blood 112:120-30
Earl, L A; Baum, L G (2008) CD45 glycosylation controls T-cell life and death. Immunol Cell Biol 86:608-15
Bi, Shuguang; Earl, Lesley A; Jacobs, Linsey et al. (2008) Structural features of galectin-9 and galectin-1 that determine distinct T cell death pathways. J Biol Chem 283:12248-58
Belitsky, Jason M; Nelson, Alshakim; Hernandez, Joseph D et al. (2007) Multivalent interactions between lectins and supramolecular complexes: Galectin-1 and self-assembled pseudopolyrotaxanes. Chem Biol 14:1140-51
Hernandez, Joseph D; Klein, Jeffrey; Van Dyken, Stephen J et al. (2007) T-cell activation results in microheterogeneous changes in glycosylation of CD45. Int Immunol 19:847-56

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