Abstract

The long-term goal of this proposal is to gain insight into the cellular and molecular mechanisms underlying B cell clonal expansion and malignant transformation in AIDS-associated non Hodgkin's lymphoma (NHL). As a result of the introduction of relatively effective anti-retroviral therapy and the consequent higher survival rate, NHLs have become important causes of pathology in AIDS patients. In these patients, most NHLs are Burkitt- type B cell lymphomas, and display features similar to those of sporadic Burkitt's lymphoma (BL) occurring in HIV-negative patients, including t(8;14), t(8;22) or t(2;8) chromosomal translocation and c-myc proto- oncogene activation. This represents an important, but not, perhaps, sufficient event in lymphomagenesis. Full malignant transformation would require either activation of a second proto-oncogene or a stochastic second event, such as infection with Epstein-Barr virus (EBV), a powerful B lymphotropic transforming agent. EBV is present in virtually all endemic (African) BLs, but it is found only in a minority of AIDS BLs, suggesting that other B cell """"""""driving"""""""" cofactors underlie the malignant transformation of these lymphocytes. This view is further supported by the generalized B cell """"""""hyperactivity"""""""", often associated with lymph node follicular hyperplasia, found in a significant proportion of AIDS patients prior to tumoral outgrowth; and by our preliminary findings showing that the variable segments of the specific anti-rd blood cell i/I antigen autoantibodies produced by two different AIDS-associated BLs bear imprints (somatic point-mutations) that are characteristic of a persistent antigenic stimulation. We hypothesize that a mechanism of self or foreign antigen-driven B cell clonal expansion and selection precedes and/or is associated with the cellular events leading to malignant transformation in AIDS BL. Conversely, antigenic stimulation may play a less important or negligible role in the emergence and/or sustenance of neoplastic B cells in the endemic variety of BL. To test our hypothesis, we propose to analyze the antigen specificity of the antibodies produced by AIDS BLs, and determine whether their variable segments contain somatic point- mutations in a fashion consistent with a process of antigen-driven clonal selection of such mutations. In addition, we propose to verify whether progenitors of the neoplastic clonotype are present among """"""""non-neoplastic"""""""" B cells, as defined by phenotypic and genotypic analysis, obtained prior to tumoral outgrowth. The molecular features of AIDS BL will be compared with those derived from the analysis of the sporadic and endemic forms of the tumor. The demonstration that a process of Ag-driven clonal expansion and selection is an important event or cofactor, along with the characteristic genetic lesions, in AIDS-associated lymphomagenesis would provide one of the first indications that the inherent function of the (immune) cells involved in the neoplastic process are crucial for tumor development, and may provide the basis for specific immune intervention.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Research Project (R01)
Project #
5R01CA068541-04
Application #
2633909
Study Section
AIDS and Related Research Study Section 3 (ARRC)
Program Officer
Finerty, John F
Project Start
1995-01-19
Project End
1998-12-31
Budget Start
1998-01-01
Budget End
1998-12-31
Support Year
4
Fiscal Year
1998
Total Cost
Indirect Cost

  Institution

Name
Weill Medical College of Cornell University
Department
Pathology
Type
Schools of Medicine
DUNS #
201373169
City
New York
State
NY
Country
United States
Zip Code
10065

  Publications

Phillips-Quagliata, J M; Faria, A M; Han, J et al. (2001) IgG2a and igA co-expression by the natural autoantibody-producing murine B lymphoma T560. Autoimmunity 33:181-97
Ikematsu, H; Cerutti, A; Zan, H et al. (2000) Ongoing hypermutation in the Ig V(D)J gene segments and c-myc proto-oncogene of an AIDS lymphoma segregates with neoplastic B cells at different sites: implications for clonal evolution. Hum Immunol 61:1242-53
Matolcsy, A; Schattner, E J; Knowles, D M et al. (1999) Clonal evolution of B cells in transformation from low- to high-grade lymphoma. Eur J Immunol 29:1253-64
Cerutti, A; Schaffer, A; Shah, S et al. (1998) CD30 is a CD40-inducible molecule that negatively regulates CD40-mediated immunoglobulin class switching in non-antigen-selected human B cells. Immunity 9:247-56
Cerutti, A; Zan, H; Schaffer, A et al. (1998) CD40 ligand and appropriate cytokines induce switching to IgG, IgA, and IgE and coordinated germinal center and plasmacytoid phenotypic differentiation in a human monoclonal IgM+IgD+ B cell line. J Immunol 160:2145-57
Schettino, E W; Cerutti, A; Chiorazzi, N et al. (1998) Lack of intraclonal diversification in Ig heavy and light chain V region genes expressed by CD5+IgM+ chronic lymphocytic leukemia B cells: a multiple time point analysis. J Immunol 160:820-30
Matolcsy, A; Casali, P; Nador, R G et al. (1997) Molecular characterization of IgA- and/or IgG-switched chronic lymphocytic leukemia B cells. Blood 89:1732-9
Matolcsy, A; Casali, P; Warnke, R A et al. (1996) Morphologic transformation of follicular lymphoma is associated with somatic mutation of the translocated Bcl-2 gene. Blood 88:3937-44
Casali, P; Schettino, E W (1996) Structure and function of natural antibodies. Curr Top Microbiol Immunol 210:167-79
Matolcsy, A; Casali, P; Knowles, D M (1995) Different clonal origin of B-cell populations of chronic lymphocytic leukemia and large-cell lymphoma in Richter's syndrome. Ann N Y Acad Sci 764:496-503

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