Abstract

The purpose of the proposed research is to gain knowledge regarding the function of the ecto enzyme, 5 prime-nucleotidase (ecto-5 prime-NT) on human B and T cells. The proposal is divided into three related projects. First, we will develop methods to separate ecto-5 prime-NT+ from ecto-5 prime-NT- lymphocytes. A monoclonal antibody will be produced after immunization of mice with 5 prime-NT purified from human placenta. Using anti-ecto-5 prime-NT antibodies, human peripheral T and B cells will be separated into ecto-5 prime-NT+ and ecto-5 prime-NT- populations by cell sorting, panning, complement mediated lysis of ecto-5 prime-NT+ cells, and/or rosetting. In the second project, we will conduct basic studies of purine metabolism in ecto-5 prime-NT+ and ecto-5 prime-NT-T cells. The ability of these two populations to proliferate in response to mitogens will be compared in purine-free medium (in which the cells must meet their purine requirements by de novo synthesis), in medium supplemented with hypoxathine (which can meet all purine requirements via salvage), and in medium supplemented with inosine 5 prime-monophosphate (which can meet all purine requirements via salvage only after conversion to inosine by ecto-5 prime-NT). We will learn whether the presence or absence of ecto-5 prime-NT activity influences the routes by which human T cells meet their purine requirements and whether ecto-5 prime-NT lymphocytes might have a selective advantage over ecto-5 prime-NT-lymphocytes in specific microenvironments such as the thymus and bone marrow where there is considerable cell death and purines might be salvaged from exogenous nucleotides. Finally, we will compare the functional capabilities of ecto-5 prime-NT+ vs. ecto-5-NT-T and B cells. The results of these experiments in combination with those of the second project will reveal whether specifc patterns of purine metabolism are adapted for specific types of lymphocyte functions; i.e., those which require proliferation as compared to those which do not. The purified populations will also be characterized for the co-expression of other cell surface antigens using commercially available monoclonal antibodies to determine whether the expression of ecto-5 prime-NT activity, in conjunction with other cell surface markers, can be used to define functional subsets of human T and B lymphocytes. Our goal is to understand the significance of the reduced numbers of ecto-5 prime-NT+ lymphocytes (and increased numbers of ecto-5 prime-NT- lymphocytes) in patients with immunodeficiency diseases.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Allergy and Infectious Diseases (NIAID)
Type
Research Project (R01)
Project #
2R01AI018220-04A1
Application #
3127756
Study Section
Immunological Sciences Study Section (IMS)
Project Start
1981-08-01
Project End
1988-08-31
Budget Start
1985-09-01
Budget End
1986-08-31
Support Year
4
Fiscal Year
1985
Total Cost
Indirect Cost

  Institution

Name
Scripps Research Institute
Department
Type
DUNS #
City
San Diego
State
CA
Country
United States
Zip Code
92037

  Publications

de Leve, Simone; Wirsdörfer, Florian; Cappuccini, Federica et al. (2017) Loss of CD73 prevents accumulation of alternatively activated macrophages and the formation of prefibrotic macrophage clusters in irradiated lungs. FASEB J 31:2869-2880
Wirsdörfer, Florian; de Leve, Simone; Cappuccini, Federica et al. (2016) Extracellular Adenosine Production by ecto-5'-Nucleotidase (CD73) Enhances Radiation-Induced Lung Fibrosis. Cancer Res 76:3045-56
Yago, Tadayuki; Tsukamoto, Hiroki; Liu, Zhenghui et al. (2015) Multi-Inhibitory Effects of A2A Adenosine Receptor Signaling on Neutrophil Adhesion Under Flow. J Immunol 195:3880-9
Coffey, Francis; Lee, Sang-Yun; Buus, Terkild B et al. (2014) The TCR ligand-inducible expression of CD73 marks ?? lineage commitment and a metastable intermediate in effector specification. J Exp Med 211:329-43
Qin, Lei; Thompson, Linda F; Kuzel, Timothy M et al. (2014) Requirement of NK cells for selective A2A receptor blockade to suppress CD73+ tumor metastasis. Immunotherapy 6:19-21
Thompson, Linda F (2013) Editorial: CD73 deficiency and immune dysregulation in HIV infection: cause or effect? J Leukoc Biol 94:545-7
Tsukamoto, Hiroki; Chernogorova, Petya; Ayata, Korcan et al. (2012) Deficiency of CD73/ecto-5'-nucleotidase in mice enhances acute graft-versus-host disease. Blood 119:4554-64
Blackburn, Michael R; Thompson, Linda F (2012) Adenosine deaminase deficiency: unanticipated benefits from the study of a rare immunodeficiency. J Immunol 188:933-5
Wang, Long; Fan, Jie; Thompson, Linda F et al. (2011) CD73 has distinct roles in nonhematopoietic and hematopoietic cells to promote tumor growth in mice. J Clin Invest 121:2371-82
Haskó, György; Csóka, Balázs; Koscsó, Balázs et al. (2011) Ecto-5'-nucleotidase (CD73) decreases mortality and organ injury in sepsis. J Immunol 187:4256-67

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