Abstract

Avian reticuloendotheliosis virus (REV-T) is the most virulent of all retroviruses and rapidly induces an invariably fatal lymphoma. v-Rel is the most oncogenic member of the Rel/NF-KB family of transcription factors. The ReI/NF-KB family regulates the expression of genes involved in proliferation, apoptosis, defense and wound healing responses, and embryogenesis. The ReI/NF-KB complexes bind to DNA recognition motifs as dimers. Transformation by v-Rel is the result of differential regulation of genes normally controlled by the ReI/NF-KB family. In the nuclei of transformed cells, v-Rel exists as homodimers or in heterodimers with c-ReI, NF-KBl, and NF-KB2. Since the appearance of v-Relheterodimers in the nucleus temporally correlates with an increase in the rate of cell proliferation, the association of v-Rel with endogenous ReI/NF-KB family members is likely to play a critical role in its transforming ability. We have isolated point mutants of v-Rel which have lost their ability to associate with specific ReI/NF-KB family members and propose to employ these point mutants to determine which ReI/NF-KB family members enable v-Rel to transform. The overexpression of v-Rel, results in the elevated expression of c-fos and c-jun and in repressed expression of fra-2 in fibroblast cultures and lymphoid cells. c-jun has been shown to be directly transcriptionally upregulated by v-ReI. Co-infection or sequential infection of fibroblast cultures or lymphoid cells with retroviruses expressing v-rel and a transdominant negative mutant of AP-1 activity, supjun-1, resulted in a reduction of the transformation efficiency of v-Rel. These studies did not define the role of individual AP-1 family members. The role of c-Jun, c-fos, and fra-2 in v-Rel-mediated transformation will be examined. We also propose to determine whether v-Rel directly regulates the differential expression of c-fos and fra-2. Recently, we have found that TClO, a member of the Rho family of small GTPases, is upregulated in v-Rel transformed fibroblasts. Since TCIO and other Rho proteins have been implicated in the organization of the actin cytoskeleton, it is possible that the TC1O-mediated signal transduction pathway may be responsible for the cytoskeletal remodeling observed in fibroblast transformation by v-Rel. In addition, TCIO activates c-Jun N-terminal kinase (JNK) which phosphorylates and activates c-Jun. v-Rel may, therefore, regulate AP-1 activity not only at the transcriptional level, but also at the post-translational level through the TC1O activation pathway. The last aim of this proposal is to determine if TCIO plays a role in v-ReI-mediated transformation.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Research Project (R01)
Project #
5R01CA033192-18
Application #
6632899
Study Section
Virology Study Section (VR)
Program Officer
Read-Connole, Elizabeth Lee
Project Start
1984-01-01
Project End
2005-06-30
Budget Start
2003-07-01
Budget End
2004-06-30
Support Year
18
Fiscal Year
2003
Total Cost
$298,223
Indirect Cost

  Institution

Name
University of Texas Austin
Department
Biology
Type
Schools of Arts and Sciences
DUNS #
170230239
City
Austin
State
TX
Country
United States
Zip Code
78712

  Publications

Hrdli?ková, Radmila; Nehyba, Ji?í; Bargmann, William et al. (2014) Multiple tumor suppressor microRNAs regulate telomerase and TCF7, an important transcriptional regulator of the Wnt pathway. PLoS One 9:e86990
Hrdlickova, Radmila; Nehyba, Jiri; Lim, Shu Ly et al. (2012) Insights into the evolution of mammalian telomerase: platypus TERT shares similarities with genes of birds and other reptiles and localizes on sex chromosomes. BMC Genomics 13:216
Hrdlickova, Radmila; Nehyba, Jiri; Bose Jr, Henry R (2012) Alternatively spliced telomerase reverse transcriptase variants lacking telomerase activity stimulate cell proliferation. Mol Cell Biol 32:4283-96
Tiwari, Richa; Bargmann, William; Bose Jr, Henry R (2011) Activation of the TGF-ýý/Smad signaling pathway in oncogenic transformation by v-Rel. Virology 413:60-71
Liss, A S; Tiwari, R; Kralova, J et al. (2010) Cell transformation by v-Rel reveals distinct roles of AP-1 family members in Rel/NF-kappaB oncogenesis. Oncogene 29:4925-37
Kralova, J; Sheely, J I; Liss, A S et al. (2010) ERK and JNK activation is essential for oncogenic transformation by v-Rel. Oncogene 29:6267-79
Nehyba, Jiri; Hrdlickova, Radmila; Bose, Henry R (2009) Dynamic evolution of immune system regulators: the history of the interferon regulatory factor family. Mol Biol Evol 26:2539-50
Hrdlickova, Radmila; Nehyba, Jiri; Bose Jr, Henry R (2009) Regulation of telomerase activity by interferon regulatory factors 4 and 8 in immune cells. Mol Cell Biol 29:929-41
Tong, S; Liss, A S; You, M et al. (2007) The activation of TC10, a Rho small GTPase, contributes to v-Rel-mediated transformation. Oncogene 26:2318-29
Hrdlickova, Radmila; Nehyba, Jiri; Liss, Andrew S et al. (2006) Mechanism of telomerase activation by v-Rel and its contribution to transformation. J Virol 80:281-95

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