Abstract

The longterm objective of this research project is to understand the maturation of resting immunocompetent B lymphocytes into actively immunoglobulin-secreting plasma cells at the cellular, biochemical, molecular and genetic levels. Currently, attention is focussed on the identity, mechanisms of action, and biological relevance of several distinct protein molecules termed B cell Maturation Factors (BMFs). BMFs are derived from several cell types in the immune system, and are able to induce, in cultured normal or tumor B cells, all of the changes thought to be part of the resting B cell to plasma cell transition. The identity of these BMFs is being pursued both by classical protein purification and by recombinant DNA cloning. Their mechanisms of action (cell surface receptors, intracellular signals, changes in Ig metabolism and cell growth, etc.) are being investigated by a combination of molecular biological, biochemical, immunological, and genetic techniques. The relevance of BMFs is being approached by studying the effects of endogenously produced or exogenously administered BMFs on both normal and BMF-unresponsive mouse strains and tumor cells in vitro and in vivo. The information gained in these studies may have medical significance for several reasons. First, a detailed understanding of the maturation of B lymphocytes to active Ig secretion, the central process of humoral immunity may lead to more specific and efficient manipulation of the immune system in normal individuals and patients with heightened (autoimmune) or depressed (immunodeficient) immune capabilities. Second, since WEHI-279 tumor B cells are an important component of this project, these studies directly address the growth and differentiation of certain B cell tumors and how these may be modified. Finally, by identifying and cloning lymphokine (BMF) structural genes in the mouse, probes will be obtained which should allow isolation of the equivalent genes and molecules in man, for eventual diagnostic or therapeutic use.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Research Project (R01)
Project #
5R01CA035845-06
Application #
3173396
Study Section
Immunobiology Study Section (IMB)
Project Start
1983-07-01
Project End
1990-05-31
Budget Start
1988-06-01
Budget End
1990-05-31
Support Year
6
Fiscal Year
1988
Total Cost
Indirect Cost

  Institution

Name
Jackson Laboratory
Department
Type
DUNS #
042140483
City
Bar Harbor
State
ME
Country
United States
Zip Code
04609

  Publications

Prasad, V S; LaFond, R E; Zhou, M et al. (1997) Upregulation of endogenous p53 and induction of in vivo apoptosis in B-lineage lymphomas of E(mu)-myc transgenic mice by deregulated c-myc transgene. Mol Carcinog 18:66-77
Prasad, V S; Temple, M J; Davisson, M T et al. (1996) Heterogeneity of B-lymphoid tumors in E mu-myc transgenic mice. Cytometry 23:131-9
Jacobsen, K A; Prasad, V S; Sidman, C L et al. (1994) Apoptosis and macrophage-mediated deletion of precursor B cells in the bone marrow of E mu-myc transgenic mice. Blood 84:2784-94
Sidman, C L; Denial, T M; Marshall, J D et al. (1993) Multiple mechanisms of tumorigenesis in E mu-myc transgenic mice. Cancer Res 53:1665-9
Sidman, C L; Shaffer, D J; Jacobsen, K et al. (1993) Cell populations during tumorigenesis in Eu-myc transgenic mice. Leukemia 7:887-95
Pilcher, J B; Tsang, V C; Zhou, W et al. (1991) Optimization of binding capacity and specificity of protein G on various solid matrices for immunoglobulins. J Immunol Methods 136:279-86
Freitas, A A; Sidman, C L (1990) VH gene family repertoires of ""viable motheaten"" (mev) mice. Eur J Immunol 20:1033-7
Allen, R D; Marshall, J D; Roths, J B et al. (1990) Differences defined by bone marrow transplantation suggest that lpr and gld are mutations of genes encoding an interacting pair of molecules. J Exp Med 172:1367-75
Allen, R D; Marshall, J D; Roths, J B et al. (1990) Bone marrow transplantation from mutant lpr/lpr mice. Functional abnormalities rather than alloantigenic differences appear to determine the development of a graft-vs.-host-like syndrome. Eur J Immunol 20:2057-66
Roths, J B; Marshall, J D; Allen, R D et al. (1990) Spontaneous Pneumocystis carinii pneumonia in immunodeficient mutant scid mice. Natural history and pathobiology. Am J Pathol 136:1173-86

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