Abstract

The specific objectives of this proposed study are: (1) to investigate the hypothesis that the T-lymphocyte transmembrane glycoprotein CD45 (GP180), closely interacts with the T cell antigen receptor/CD3 complex (TCR/CD3 complex); and to analyze the linkage between CD45(GP180) and the cytoskeleton in the T-lymphocyte plasma membrane; and (2) to identify the IP3 receptor on Ca2+ storage vesicles (calciosomes) responsible for IP3- induced internal CA2+ release during lymphocyte activation. The employment of complementary techniques including density perturbation technique [for CD45(GP180) patch/cap isolation], non-ionic detergent extraction (e.g. Triton X-114) and Con A-Sepharose column chromatography should allow us to isolate the putative CD45 (GP180)-TCR/CD3 complex and identify substrates of the CD45 (GP180)-tyrosine phosphatase in these receptor complexes as well as the relevant CD45(GP180)-cytoskeleton complexes. The proposed experiments concerning reconstitution of CD45(GP180) into liposomes (phospholipid vesicles) will allow us to directly examine any direct interactions which occur between CD45(GP180) and various cytoskeletal components. Furthermore, the experiments proposed to test the effect of the cytoskeleton on CD45(GP180)-associated tyrosine phosphatase activity should provide new insights concerning the regulatory role of the cytoskeleton in signal transduction. In addition, we propose to identify the IP3 receptor on Ca2+ storage vesicles (calciosomes) responsible for IP3-induced internal Ca2+ release during lymphocyte activation. A variety of methods including cellular fractionation, density gradient centrifugation, radiolabel binding assays, CA2+ flux measurements and immunocytochemistry, will be used to analyze both the IP3 receptor and IP3-induced internal Ca2+ release mechanism which is required for the onset of lymphocyte activation by a specific ligands (e.g. anti-TCR or anti-CD3 antibodies). We believe that the proposed experiments will allow us to obtain valuable new insight(s) concerning (a) the relationships between CD45 (GP180) and TCR/CD3 complex during T-cell activation; (b) the functional role of the cytoskeleton in regulating signal transducing systems (e.g. tyrosine phosphatase activity); and (c) the molecular and cellular mechanisms involved in regulating internal Ca2+ release from intracellular storage sites. This knowledge is critically needed to further our understanding of lymphocyte activation during various immunological reactions and certain immunodeficiency-related diseases.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of General Medical Sciences (NIGMS)
Type
Research Project (R01)
Project #
5R01GM036353-11
Application #
3290155
Study Section
Immunobiology Study Section (IMB)
Project Start
1982-01-01
Project End
1995-06-30
Budget Start
1992-07-01
Budget End
1993-06-30
Support Year
11
Fiscal Year
1992
Total Cost
Indirect Cost

  Institution

Name
University of Miami School of Medicine
Department
Type
Schools of Medicine
DUNS #
City
Miami
State
FL
Country
United States
Zip Code
33146

  Publications

Iida, N; Bourguignon, L Y (1997) Coexpression of CD44 variant (v10/ex14) and CD44S in human mammary epithelial cells promotes tumorigenesis. J Cell Physiol 171:152-60
Donnadieu, E; Bourguignon, L Y (1996) Ca2+ signaling in endothelial cells stimulated by bradykinin: Ca2+ measurement in the mitochondria and the cytosol by confocal microscopy. Cell Calcium 20:53-61
Lokeshwar, V B; Iida, N; Bourguignon, L Y (1996) The cell adhesion molecule, GP116, is a new CD44 variant (ex14/v10) involved in hyaluronic acid binding and endothelial cell proliferation. J Biol Chem 271:23853-64
Zhu, D; Bourguignon, L (1996) Overexpression of CD44 in pl85(neu)-transfected NIH3T3 cells promotes an up-regulation of hyaluronic acid-mediated membrane-cytoskeleton interaction and cell adhesion. Oncogene 12:2309-14
Peck, M D; Li, Z; Jy, W et al. (1996) Association of murine splenocyte CD3 complex to the cytoskeleton: absence of modulation by exogenous fatty acids. Cell Biol Int 20:531-7
Iida, N; Bourguignon, L Y (1995) New CD44 splice variants associated with human breast cancers. J Cell Physiol 162:127-33
Bourguignon, L Y; Chu, A; Jin, H et al. (1995) Ryanodine receptor-ankyrin interaction regulates internal Ca2+ release in mouse T-lymphoma cells. J Biol Chem 270:17917-22
Welsh, C F; Zhu, D; Bourguignon, L Y (1995) Interaction of CD44 variant isoforms with hyaluronic acid and the cytoskeleton in human prostate cancer cells. J Cell Physiol 164:605-12
Bourrguignon, L Y; Iida, N; Welsh, C F et al. (1995) Involvement of CD44 and its variant isoforms in membrane-cytoskeleton interaction, cell adhesion and tumor metastasis. J Neurooncol 26:201-8
Lokeshwar, V B; Fregien, N; Bourguignon, L Y (1994) Ankyrin-binding domain of CD44(GP85) is required for the expression of hyaluronic acid-mediated adhesion function. J Cell Biol 126:1099-109

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