Abstract

Interference with differentiation is a major step in tumor progression. In myeloid cells deregulated expression of c-Myc blocks terminal differentiation, promoting both proliferation and an apoptotic response associated with the block in differentiation. The Myc mutants mycS and T58A each block myeloid differentiation without the apoptotic response, possibly being more aggressive oncogenes than wild type c-myc in myeloid cells. Eliminating Gadd45 expression influences the response of myeloid cells to deregulated Myc by eliminating the apoptotic response associated with the Myc-mediated block in differentiation; therefore Gadd45 genes behave as tumor suppressors. Acceleration of tumorigenesis in transgenic mouse models is observed when apoptosis is suppressed. Thus, it is hypothesized that the response of myeloid cells to deregulated Myc expression depends not only on the genetic status of Myc, but also on the status of the other genes expressed in the cell, including the Gadd45 family of genes. It is further hypothesized that the initial response of myeloid cells to c-Myc will have ramifications not only on how the cells respond to differentiation signals, but also long term effects with regard to proliferation and eventually leukemic transformation. Accordingly, three specific aims are proposed.
Aim I : Dissect the c-Myc Block in Terminal Differentiation and Its Associated Apoptosis Using c-Myc Mutant Proteins.
Aim II : Analyze the Effect of Deregulated Expression of c-Myc in Myeloid Cells Deficient in Gadd45.
Aim III : Identify and Assess the Role of Different c-Myc Target Genes, Including Gadd45b and Gadd45g, in Blocking Myeloid Differentiation and Activating Premature Apoptosis. These studies will lead to a greater understanding of how c-Myc participates in the neoplastic process by influencing proliferation rates. It will encompass how mutations in either c-Myc itself or in cellular genes, specifically the Gadd45 gene family, suppresses the Myc-mediated apoptotic response associated with the block in myeloid differentiation, enhancing the leukemic potential of c-Myc. This knowledge should provide novel tools for designing drugs to promote differentiation and/or apoptosis of leukemic cells.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Research Project (R01)
Project #
5R01CA081168-08
Application #
7247261
Study Section
Tumor Cell Biology Study Section (TCB)
Program Officer
Mufson, R Allan
Project Start
1999-04-01
Project End
2010-06-30
Budget Start
2007-07-01
Budget End
2008-06-30
Support Year
8
Fiscal Year
2007
Total Cost
$272,010
Indirect Cost

  Institution

Name
Temple University
Department
Biochemistry
Type
Schools of Medicine
DUNS #
057123192
City
Philadelphia
State
PA
Country
United States
Zip Code
19122

  Publications

Maifrede, Silvia; Magimaidas, Andrew; Sha, Xiaojin et al. (2017) Loss of Egr1, a human del5q gene, accelerates BCR-ABL driven chronic myelogenous leukemia. Oncotarget 8:69281-69294
Salerno, Dominic M; Tront, Jennifer S; Hoffman, Barbara et al. (2012) Gadd45a and Gadd45b modulate innate immune functions of granulocytes and macrophages by differential regulation of p38 and JNK signaling. J Cell Physiol 227:3613-20
Liebermann, Dan A; Tront, Jennifer S; Sha, Xiogen et al. (2011) Gadd45 stress sensors in malignancy and leukemia. Crit Rev Oncog 16:129-40
Cretu, Alexandra; Sha, Xiaojin; Tront, Jennifer et al. (2009) Stress sensor Gadd45 genes as therapeutic targets in cancer. Cancer Ther 7:268-276
Liebermann, Dan A; Hoffman, Barbara (2009) Good and bad IRF-1: role in tumor suppression versus autoimmune disease. Leuk Res 33:1301-2
Zumbrun, Steven D; Hoffman, Barbara; Liebermann, Dan A (2009) Distinct mechanisms are utilized to induce stress sensor gadd45b by different stress stimuli. J Cell Biochem 108:1220-31
Gibbs, J D; Liebermann, D A; Hoffman, B (2008) Leukemia suppressor function of Egr-1 is dependent on transforming oncogene. Leukemia 22:1909-16
Gibbs, J D; Liebermann, D A; Hoffman, B (2008) Egr-1 abrogates the E2F-1 block in terminal myeloid differentiation and suppresses leukemia. Oncogene 27:98-106
D'Angelo, Santo; Liebermann, Dan; Hoffman, Barbara (2008) The c-myc apoptotic response is not intrinsic to blocking terminal myeloid differentiation. J Cell Physiol 216:120-7
Hoffman, Barbara; Liebermann, Dan A (2007) Role of gadd45 in myeloid cells in response to hematopoietic stress. Blood Cells Mol Dis 39:344-7

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