Abstract

Genes encoding transcription factors are the targets of specific chromosomal translocations in human leukemic cells, but the mechanisms by which they promote aberrant growth and differentiation are still largely undefined. This proposal focuses on hepatic leukemia factor (HLF), a newly identified sequence-specific DNA-binding protein of the basic-region/leucine-zipper (bZip) superfamily. A t(17;19)(q22;pl3) chromosomal translocation in childhood B-lineage acute lymphoblastic leukemia (ALL) disrupts the HLF gene at the breakpoint on chromosome 17 and the E2A gene at the breakpoint on chromosome 19. The resulting fusion gene (E2A-HLF) produces chimeric proteins that retain the amino-terminal transcriptional activation domain of E2A, but not its basic helix-loop-helix domain, which is replaced by the bZip DNA-binding and dimerization domain of the HLF protein. An attractive hypothesis to account for productive E2A-HLF gene rearrangements in cases of early B-lineage ALL is that the chimeric proteins contribute to malignant transformation and ensure maintenance of the leukemic state. The proposed research will be conducted on two distinct but complementary aspects of the roles of HLF and E2A-HLF proteins in the pathogenesis of childhood acute leukemia. First, the ability of E2A-HLF and HLF proteins to regulate the expression of reporter genes in constructs containing cis-acting DNA sequences that mediate HLF binding will be tested in lymphoid and myeloid leukemia cell lines. These studies will also assess the ability of HLF to heterodimerize with other bZip proteins, in order to determine whether homo- or heterodimers of normal or chimeric HLF proteins activate the expression of critical target genes in leukemic cells. Concurrently, the oncogenic potential and spectrum of progenitor cells susceptible to the transforming effects of these proteins will be determined in murine bone marrow cells infected with retroviral vectors carrying E2A-HLF or HLF cDNAs. Functional domains of chimeric E2A-HLF proteins will be tested separately, to determine how this hybrid protein can subvert the transcriptional programs that normally control the growth and differentiation of hematopoietic cells. Improved understanding of the involvement of these transcription factors in human acute leukemias should yield important information about the regulatory circuits governing normal hematopoiesis and may suggest new approaches for the diagnosis and treatment of hematopoietic malignancies.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Research Project (R01)
Project #
5R01CA059571-02
Application #
2100163
Study Section
Hematology Subcommittee 2 (HEM)
Project Start
1993-05-01
Project End
1998-02-28
Budget Start
1994-05-01
Budget End
1995-02-28
Support Year
2
Fiscal Year
1994
Total Cost
Indirect Cost

  Institution

Name
St. Jude Children's Research Hospital
Department
Type
DUNS #
067717892
City
Memphis
State
TN
Country
United States
Zip Code
38105

  Publications

Wu, Wen-Shu; Heinrichs, Stefan; Xu, Dong et al. (2005) Slug antagonizes p53-mediated apoptosis of hematopoietic progenitors by repressing puma. Cell 123:641-53
Ferrando, Adolfo A; Look, A Thomas (2003) Gene expression profiling in T-cell acute lymphoblastic leukemia. Semin Hematol 40:274-80
Inoue, Akira; Seidel, Markus G; Wu, Wenshu et al. (2002) Slug, a highly conserved zinc finger transcriptional repressor, protects hematopoietic progenitor cells from radiation-induced apoptosis in vivo. Cancer Cell 2:279-88
Dang, J; Inukai, T; Kurosawa, H et al. (2001) The E2A-HLF oncoprotein activates Groucho-related genes and suppresses Runx1. Mol Cell Biol 21:5935-45
Ferrando, A A; Look, A T (2000) Clinical implications of recurring chromosomal and associated molecular abnormalities in acute lymphoblastic leukemia. Semin Hematol 37:381-95
Hitzler, J K; Soares, H D; Drolet, D W et al. (1999) Expression patterns of the hepatic leukemia factor gene in the nervous system of developing and adult mice. Brain Res 820:1-11
Kurosawa, H; Goi, K; Inukai, T et al. (1999) Two candidate downstream target genes for E2A-HLF. Blood 93:321-32
Kuribara, R; Kinoshita, T; Miyajima, A et al. (1999) Two distinct interleukin-3-mediated signal pathways, Ras-NFIL3 (E4BP4) and Bcl-xL, regulate the survival of murine pro-B lymphocytes. Mol Cell Biol 19:2754-62
Inukai, T; Inoue, A; Kurosawa, H et al. (1999) SLUG, a ces-1-related zinc finger transcription factor gene with antiapoptotic activity, is a downstream target of the E2A-HLF oncoprotein. Mol Cell 4:343-52
Inukai, T; Inaba, T; Ikushima, S et al. (1998) The AD1 and AD2 transactivation domains of E2A are essential for the antiapoptotic activity of the chimeric oncoprotein E2A-HLF. Mol Cell Biol 18:6035-43

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