Abstract

Our research goal is to understand the molecular structure and function of the genes that play critical roles in normal growth and differentiation, neoplastic transformation, and apoptosis in mouse and human tissues and tumors. We study oncogenes, particularly c-myc, v-raf, v-abl and v- and c-cbl; anti-oncogenes, esp. the cell cycle-regulating proteins (cyclins) and their inhibitors, p21 (waf) and p16; the bcl-2 family; as well as molecules that transduce signals within the cell, esp., protein kinase C (PKC). We and others have shown that the deregulated expression of c-myc secondary to chromosomal translocations in the c-myc region is an essential element in the series of genetic alterations that are involved in plasmacytomagenesis in BALB/c mice and in Burkitt and AIDS-associated lymphomas in man. It is not known why BALB/c mice are particularly susceptible to these genetic aberratons, but we have a candidate mechanism. We have found that the BALB/c mouse has an unusual defect in a special form of excision repair of DNA damage. This form of excision repair is unusual in that, unlike most forms of DNA excision repair it is not coupled to RNA transcription. Furthermore, the defect is only manifest in repair of DNA damage in the c-myc, Pvt1, switch Ig a and Ig k genes, namely the sites of recurrent chromosomal translocations in B-lymphocytic neoplasms. This is a plausible mechanism for the production of the gene- specific, strain-specific genomic instability that predisposes BALB/c mice to the chromosome translocations that lead to constitutive expression of c-myc. This dysregulated expression of c-myc, in turn, leads to an extension of gene-specific genetic instability to a new subset of genes, including cyclin D2, RNR2 (subunit 2 of ribonucleotide reductase) and dihydro- folate reductase (dhfr). This subset of genes uniquely becomes amplified and overexpressed as a response to c-myc overexpression, possibly contributing to uncontrolled cell proliferation. We have cloned eight Protein Kinase C (PKC) isozymes into a variety of expression vectors and produced cell lines that overexpress each of these isoforms. We have also produced chimeric PKC molecules, i.e., half PKC-d and half PKC-e, and cell lines that overexpress them, to determine whether the regulatory half or the catalytic half controls various functions of PKC. PKC-d is able to mediate TPA-induced macrophage differentiation of promyelocytes, while overexpression of PKC-e in rodent fibroblasts is transforming in vitro and tumorigenic in vivo. Overexpression of the PKC chimeras showed that the C-terminal half, containing the catalytic domain, appears to bear most of the isoform- specific determinants of myeloid differentiation and fibroblast transformation.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Intramural Research (Z01)
Project #
1Z01BC008727-20
Application #
6100922
Study Section
Special Emphasis Panel (LG)
Project Start
Project End
Budget Start
Budget End
Support Year
20
Fiscal Year
1998
Total Cost
Indirect Cost

  Institution

Name
National Cancer Institute Division of Basic Sciences
Department
Type
DUNS #
City
State
Country
United States
Zip Code

  Publications

Park, Eun Sung; Lee, Ju-Seog; Woo, Hyun Goo et al. (2007) Heterologous tissue culture expression signature predicts human breast cancer prognosis. PLoS One 2:e145
Wang, Hongyang; Owens, James D; Shih, Joanna H et al. (2006) Histological staining methods preparatory to laser capture microdissection significantly affect the integrity of the cellular RNA. BMC Genomics 7:97
Thiefes, Axel; Wolter, Sabine; Mushinski, J Frederic et al. (2005) Simultaneous blockade of NFkappaB, JNK, and p38 MAPK by a kinase-inactive mutant of the protein kinase TAK1 sensitizes cells to apoptosis and affects a distinct spectrum of tumor necrosis factor [corrected] target genes. J Biol Chem 280:27728-41
Park, Sung Sup; Kim, Joong Su; Tessarollo, Lino et al. (2005) Insertion of c-Myc into Igh induces B-cell and plasma-cell neoplasms in mice. Cancer Res 65:1306-15
Romanova, Larisa Y; Hashimoto, Shigeru; Chay, Kee-Oh et al. (2004) Phosphorylation of paxillin tyrosines 31 and 118 controls polarization and motility of lymphoid cells and is PMA-sensitive. J Cell Sci 117:3759-68
Wang, Qiming Jane; Lu, Ganwei; Schlapkohl, Walter A et al. (2004) The V5 domain of protein kinase C plays a critical role in determining the isoform-specific localization, translocation, and biological function of protein kinase C-delta and -epsilon. Mol Cancer Res 2:129-40
Mai, Sabine; Mushinski, J Frederic (2003) c-Myc-induced genomic instability. J Environ Pathol Toxicol Oncol 22:179-99
Kim, J S; Pirnia, F; Choi, Y H et al. (2000) Lovastatin induces apoptosis in a primitive neuroectodermal tumor cell line in association with RB down-regulation and loss of the G1 checkpoint. Oncogene 19:6082-90
Kuschak, T I; Taylor, C; McMillan-Ward, E et al. (1999) The ribonucleotide reductase R2 gene is a non-transcribed target of c-Myc-induced genomic instability. Gene 238:351-65
Romanova, L Y; Alexandrov, I A; Blagosklonny, M V et al. (1999) Regulation of actin cytoskeleton in lymphocytes: PKC-delta disrupts IL-3-induced membrane ruffles downstream of Rac1. J Cell Physiol 179:157-69

Showing the most recent 10 out of 12 publications