Abstract

Proto-oncogene c-abl is a normal constituent of the vertebrate genomes. Three lines of evidence indicate the importance of this gene in the regulation of cell growth and development: (a) viral derivatives of the c-abl gene can induce cancers in mice and cats; (b) human c-abl gene is consistently translocated in the Philadelphia chromosome of chronic myclogenous leukemia to generate an altered c-abl proteins; (c) the expression of c-abl gene is modulated during embryogenesis and spermatogenesis. Our research goals are to elucidate the normal function of c-able and to understand the mechanism of tumorogenesis induced by the oncogenic derivatives of the c-abl gene. We have succeeded in isolating cDNA clones of the normal c-abl RNA, monoclonal antibodies that reach with the c-abl proteins and antibodies that recognize phosphotyrosine. The analyses of our cDNA clones revealed an unexpected finding that several RNAs with different 5'-sequences are generated from the mouse c-abl gene. In this proposal, we will determine the 5'-structure of the c-abl gene and the molecular mechanism for the generation of the heterogeneous c-abl RNAs. We will examine the possible regulation of the expression of these RNAs by tumorogenic processes, by development, and by mitogenic stimulation. The heterogenous regions of these c-abl RNAs contain protein coding sequences. We will define the protein product of each of these RNAs in vitro. Each of the c-abl cDNAs will be expressed in mouse cells at high levels so that the properties and the enzymatic activity of the cellular c-abl proteins can be analyzed. We will study the tyrosine kinase activity of the c-abl proteins; compare them to the oncogenic v-abl protein; and examine the regulation of the c-abl tyrosine kinase activity in mouse cells and in a bacterial expression system. The analyses of the c-abl tyrosine kinase activity, which is crucial to the function of the c-abl protein, will be facilitated by the anti-phosphotyrosine antibodies we have isolated. The proposed studiew will define the structure of the c-abl gene, the regulation of the generation of different c-abl RNAs and the structures and enzymatic functions of the c-abl proteins. These results will form the basis for future studies leading to the understanding of c-abl gene function in cell growth and differentiation.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Research Project (R01)
Project #
5R01CA043054-03
Application #
3184920
Study Section
Molecular Biology Study Section (MBY)
Project Start
1986-08-01
Project End
1989-07-31
Budget Start
1988-08-01
Budget End
1989-07-31
Support Year
3
Fiscal Year
1988
Total Cost
Indirect Cost

  Institution

Name
University of California San Diego
Department
Type
Schools of Arts and Sciences
DUNS #
077758407
City
La Jolla
State
CA
Country
United States
Zip Code
92093

  Publications

Rastogi, Shubhra; Hwang, Amini; Chan, Josolyn et al. (2018) Extracellular vesicles transfer nuclear Abl-dependent and radiation-induced miR-34c into unirradiated cells to cause bystander effects. Mol Biol Cell 29:2228-2242
Zhou, Yuanshuai; Xu, Zhongjuan; Quan, Daniel et al. (2018) Nuclear respiratory factor 1 promotes spheroid survival and mesenchymal transition in mammary epithelial cells. Oncogene :
Tu, Chi-Chiang; Wang, Jean Y J (2016) EnABLing microprocessor for apoptosis. Mol Cell Oncol 3:
Hu, Wan-Hsiang; Miyai, Katsumi; Sporn, Judith C et al. (2016) Loss of histone variant macroH2A2 expression associates with progression of anal neoplasm. J Clin Pathol 69:627-31
Tonino, Sanne H; Mulkens, Chantal E; van Laar, Jacoline et al. (2015) Induction of TAp73 by platinum-based compounds to overcome drug resistance in p53 dysfunctional chronic lymphocytic leukemia. Leuk Lymphoma 56:2439-47
Suknuntha, Kran; Ishii, Yuki; Tao, Lihong et al. (2015) Discovery of survival factor for primitive chronic myeloid leukemia cells using induced pluripotent stem cells. Stem Cell Res 15:678-693
Pineda, Gabriel; Shen, Zhouxin; de Albuquerque, Claudio Ponte et al. (2015) Proteomics studies of the interactome of RNA polymerase II C-terminal repeated domain. BMC Res Notes 8:616
Ishii, Yuki; Nhiayi, May Keu; Tse, Edison et al. (2015) Knockout Serum Replacement Promotes Cell Survival by Preventing BIM from Inducing Mitochondrial Cytochrome C Release. PLoS One 10:e0140585
Tu, Chi-Chiang; Zhong, Yan; Nguyen, Louis et al. (2015) The kinase ABL phosphorylates the microprocessor subunit DGCR8 to stimulate primary microRNA processing in response to DNA damage. Sci Signal 8:ra64
Manthey, Carolin F; Calabio, Christine B; Wosinski, Anna et al. (2014) Indispensable functions of ABL and PDGF receptor kinases in epithelial adherence of attaching/effacing pathogens under physiological conditions. Am J Physiol Cell Physiol 307:C180-9

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