Abstract

Several of the most central, unsolved problems of immunobiology are how T-lymphocyte commitment, diversification and function arise during development. In a variety of developmental systems, such processes are associated with the accumulation of lineage-specific mRNAs and their protein products. Recently developed molecular approaches have provided the means by which to isolate, identify and study the expression and function of these developmentally important macromolecules. Based on this information, at least two experimentally testable hypotheses can be proposed regarding T-cell lineage commitment and maturation. 1. That there are multiple and as yet undescribed proteins encoded by lineage-specific mRNAs that accompany early commitment of cells to the T-cell lineage during development. 2. That there is a programmed, differential expression of such lineage-specific mRNAs in diverging cell types representing distinct stages in T-cell maturation and functional diversification. The first hypothesis will be approached by attempting to isolate such lineage-specific mRNAs from different developmental stages of thymocytes using the methods of subscription hybridization and cDNA cloning. The second hypothesis will be tested by mapping the expression patterns of lineage-specific mRNAs by in situ hybridization alone and in combination with immunocytologic staining. In further support of these studies and to provide a system in which to further study the expression and function of T- cell lineage-specific mRNAs and their encoded products, T-cell hybridomas will be generated from different organs during development to permit the clonal expansion of cultured cells that demonstrate stage-specific expression of lineage-restricted mRNAs. Such studies should significantly add to our understanding of the mRNAs and their products that accompany T-cell lineage commitment and diversification and thus to our knowledge of the development of host defense. The elucidation of such processes are furthermore central to any fundamental understanding of a variety of inherited immune deficiency diseases as well as how immune reconstitution occurs following bone marrow transplantation. Finally, the identification of such lineage-specific mRNAs and their expression patterns may provide a very useful approach to better classification of lymphoid malignancies.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of General Medical Sciences (NIGMS)
Type
First Independent Research Support & Transition (FIRST) Awards (R29)
Project #
5R29GM038156-03
Application #
3466161
Study Section
Immunobiology Study Section (IMB)
Project Start
1987-07-01
Project End
1992-06-30
Budget Start
1989-07-01
Budget End
1990-06-30
Support Year
3
Fiscal Year
1989
Total Cost
Indirect Cost

  Institution

Name
Dana-Farber Cancer Institute
Department
Type
DUNS #
149617367
City
Boston
State
MA
Country
United States
Zip Code
02115

  Publications

Cao, B N; Huneycutt, B S; Gapud, C P et al. (1993) Lymphokine expression profile of resting and stimulated CD4+ CTL clones specific for the glycoprotein of vesicular stomatitis virus. Cell Immunol 146:147-56
Arceci, R J; Pampfer, S; Pollard, J W (1992) Expression of CSF-1/c-fms and SF/c-kit mRNA during preimplantation mouse development. Dev Biol 151:1-8
Maziarz, R T; Arceci, R J; Bernstein, S C et al. (1992) A gamma delta+ T-cell leukemia bearing a novel t(8;14)(q24;q11) translocation demonstrates spontaneous in vitro natural killer-like activity. Blood 79:1523-31
Arceci, R J; Stieglitz, K; Bierer, B E (1992) Immunosuppressants FK506 and rapamycin function as reversal agents of the multidrug resistance phenotype. Blood 80:1528-36
Pampfer, S; Arceci, R J; Pollard, J W (1991) Role of colony stimulating factor-1 (CSF-1) and other lympho-hematopoietic growth factors in mouse pre-implantation development. Bioessays 13:535-40
Arceci, R J; Baas, F; Raponi, R et al. (1990) Multidrug resistance gene expression is controlled by steroid hormones in the secretory epithelium of the uterus. Mol Reprod Dev 25:101-9
Croop, J M; Raymond, M; Haber, D et al. (1989) The three mouse multidrug resistance (mdr) genes are expressed in a tissue-specific manner in normal mouse tissues. Mol Cell Biol 9:1346-50
Sen, J; Arceci, R J; Jones, W et al. (1989) Expression and ontogeny of murine CD2. Eur J Immunol 19:1297-302
Greenberger, L M; Croop, J M; Horwitz, S B et al. (1989) P-glycoproteins encoded by mdr 1b in murine gravid uterus and multidrug resistant tumor cell lines are differentially glycosylated. FEBS Lett 257:419-21
Wimperis, J Z; Niemeyer, C M; Sieff, C A et al. (1989) Granulocyte-macrophage colony-stimulating factor and interleukin-3 mRNAs are produced by a small fraction of blood mononuclear cells. Blood 74:1525-30

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