Abstract

Follicular lymphoma is one of the few slowly progressing malignancies where disease evolution can be followed through repeated biopsies. In a study of 156 patients, we have observed that the majority of patients with follicular lymphoma and some with diffuse large cell lymphoma have a characteristic t(14;18)(q32.3;q21.3) chromosome translocation with a bcl- 2/IgH gene rearrangement. In addition, 1 to 8 of the 20 additional recurrent chromosome defects were noticed during disease evolution. Some, such as duplication 2p and 3p, correlated with cell phenotype or aggressiveness. In a few cases we and others have found a combined t(14;18) and either t(8;14) or t(8;17) with bcl-2 and c-myc rearrangements. More prevalent chromosomal sites involved in rearrangement include 1p36, 2p13, 3q27, 6q21 and 17q21. The oncogenes fgr, lck, re1, fim-3, myb, ros, fyn and bcl-3, have been mapped to these regions. We plan to use Southern and Northern blot analysis, pulsed field gel electrophoresis and molecular cloning, to determine whether some of these genes are altered during the course of the disease. To this effect, we have prepared genomic libraries from lymphoma samples containing either t(3;14)(q27;q32.3) or t(14;17)(q32.1;q21) to identify the genes affected by these rearrangements. Southern blot analysis of a patient with 2p13 rearrangements suggest that the c-rel oncogene, which has not previously been implicated in human neoplasia, may be the primary gene affected in this region. We have found suggestive evidence of c-rel rearrangement or amplification in seven patients with follicular lymphoma and in one cell line derived from a diffuse large cell lymphoma with inv ins(2;2)(p13;p15p11.2). All patients had very aggressive disease. In the lymphoma cell line, Southern and Northern blot analysis, as well as genomic and cDNA cloning, show that the c-rel oncogene has been truncated at the C-terminus and a hybrid c-rel message produced. DNA sequencing of the breakpoint and the fusion message, followed by expression assays, are planned. Our long range goal is to extend these types of studies to other recurrent breakpoints in order to molecularly characterize the sequential alterations leading to tumor progression, using follicular lymphoma as a model.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Research Project (R01)
Project #
7R01CA033314-13
Application #
3171242
Study Section
Pathology B Study Section (PTHB)
Project Start
1989-07-01
Project End
1995-12-31
Budget Start
1993-07-21
Budget End
1993-12-31
Support Year
13
Fiscal Year
1993
Total Cost
Indirect Cost

  Institution

Name
Thomas Jefferson University
Department
Type
Schools of Medicine
DUNS #
061197161
City
Philadelphia
State
PA
Country
United States
Zip Code
19107

  Publications

Viswanathan, M; Yu, M; Mendoza, L et al. (1996) Cloning and transcription factor-binding sites of the human c-rel proto-oncogene promoter. Gene 170:271-6
Zhang, Y; Yunis, J J (1995) Improved blood RNA extraction microtechnique for RT-PCR. Biotechniques 18:788-90, 792
Yunis, J J; Tanzer, J (1993) Molecular mechanisms of hematologic malignancies. Crit Rev Oncog 4:161-90
Thompson, J D; Brodsky, I; Yunis, J J (1992) Molecular quantification of residual disease in chronic myelogenous leukemia after bone marrow transplantation. Blood 79:1629-35
Yunis, J J; Thompson, J D (1991) Transcription regulators altered in hematologic malignancy. Nouv Rev Fr Hematol 33:92-6
Yunis, J J; Mayer, M G; Arnesen, M A et al. (1989) bcl-2 and other genomic alterations in the prognosis of large-cell lymphoma. N Engl J Med 320:1047-54
Yunis, J J (1988) Chromosomal translocations and gene rearrangements in non-Hodgkin lymphomas. Cancer Detect Prev 12:291-6
Yunis, J J (1987) Multiple recurrent genomic rearrangements and fragile sites in human cancer. Somat Cell Mol Genet 13:397-403
Yunis, J J; Frizzera, G; Oken, M M et al. (1987) Multiple recurrent genomic defects in follicular lymphoma. A possible model for cancer. N Engl J Med 316:79-84
Yunis, J J; Soreng, A L; Bowe, A E (1987) Fragile sites are targets of diverse mutagens and carcinogens. Oncogene 1:59-69

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