Abstract

Cyclin E1 (CycE) represents an essential regulator of the mammalian cell cycle and DNA replication. Our studies have recently uncovered its new role in the cell survival of hematopoietic tumor cells. We found that CycE is cleaved proteolytically during apoptosis induced by typical genotoxic agents such as ionizing radiation. This cleavage is dramatic as it affects most cellular CycE and is characteristic to all human tumor hematopoietic cells we have examined, both established cell lines or primary, freshly isolated from human patients. This cleavage is important for apoptosis as expression of a cleavage-resistant CycE mutant blocks this process. CycE cleavage generates p18CycE, which is unable to bind Cdk2 or other known interactors of CycE. Our hypothesis, supported by preliminary data, is that CycE function is mediated by its interaction with Ku70, which we have identified as a novel p18CycE-binding partner. By binding to Ku70, p18CycE1 displaces Bax, leading to its activation. Indeed, p18CycE genesis coincides with Bax activation and loss of mitochondrial functions and the ensuing apoptosis is dependent on both Bax and Ku70, since it is prevented in cells rendered deficient in these proteins by knockout or siRNA-mediated knock-down. As Ku70 is a critical component of the nonhomologous end joining (NHEJ) DNA repair, our preliminary data indicate that the CycE fragment also affects the response to DNA damage and its repair. We will determine the mechanism by which p18CycE regulates apoptosis and DNA repair, in addition to inactivating CycE function. These studies are focused on a molecule that is unique in regulating all three responses to genotoxic stress: cell cycle control, DNA repair, and apoptosis. Our objective is to understand the regulation of CycE and derivative p18CycE following genotoxic stress and their impact on cells with differential radiation sensitivity. We seek to determine: 1) how the Ku70 interaction with p18CycE regulates cell survival, 2) the regulation and role of p18CycE1, 3) the therapeutic potential of p18CycE1. These investigations will establish the contribution to apoptosis of CycE1 independent of Cdk2. Our studies will increase our understanding of the mechanism by which CycE may provide a molecular switch by coordinating key responses to genotoxic stress, that include cell cycle control, DNA repair, and apoptosis that govern the radio- or chemotherapy-induced signals in clinical therapy.

Public Health Relevance

Conversion of CycE1 to p18CycE1 is unique as it impacts on all key responses to genotoxic stress: cell proliferation, apoptosis, and DNA repair. Moreover, CycE1 is not converted to p18CycE1 in lymphocytes from normal individuals or in human epithelial or fibroblast cells. These investigations of p18CycE1 function in the absence of its Cdk2-dependent cell cycle and DNA replication regulatory function will contribute to our understanding of the novel role it plays, through p18CycE1, in apoptosis and DNA repair. In addition, these studies provide a unique approach to uncover fundamental knowledge on the intimate connections, coordinate regulation, and a possible molecular switch regulating the response of hematopoietic cells to DNA-damaging therapeutics that involve cell cycle control, DNA repair, and apoptosis.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Research Project (R01)
Project #
5R01CA127264-04
Application #
8197137
Study Section
Radiation Therapeutics and Biology Study Section (RTB)
Program Officer
Bernhard, Eric J
Project Start
2008-12-23
Project End
2013-11-30
Budget Start
2011-12-01
Budget End
2012-11-30
Support Year
4
Fiscal Year
2012
Total Cost
$315,543
Indirect Cost
$114,268

  Institution

Name
Cleveland Clinic Lerner
Department
Other Basic Sciences
Type
Schools of Medicine
DUNS #
135781701
City
Cleveland
State
OH
Country
United States
Zip Code
44195

  Publications

Andersson, E; Kuusanmäki, H; Bortoluzzi, S et al. (2016) Activating somatic mutations outside the SH2-domain of STAT3 in LGL leukemia. Leukemia 30:1204-8
Madanat, Yazan F; Smith, Mitchell R; Almasan, Alexandru et al. (2016) Idelalisib therapy of indolent B-cell malignancies: chronic lymphocytic leukemia and small lymphocytic or follicular lymphomas. Blood Lymphat Cancer 6:1-6
Andersson, Emma I; Tanahashi, Takahiro; Sekiguchi, Nodoka et al. (2016) High incidence of activating STAT5B mutations in CD4-positive T-cell large granular lymphocyte leukemia. Blood 128:2465-2468
Choudhary, G S; Al-Harbi, S; Mazumder, S et al. (2015) MCL-1 and BCL-xL-dependent resistance to the BCL-2 inhibitor ABT-199 can be overcome by preventing PI3K/AKT/mTOR activation in lymphoid malignancies. Cell Death Dis 6:e1593
Choudhary, Gaurav S; Al-Harbi, Sayer; Almasan, Alexandru (2015) Caspase-3 activation is a critical determinant of genotoxic stress-induced apoptosis. Methods Mol Biol 1219:1-9
Chatterjee, Payel; Choudhary, Gaurav S; Alswillah, Turkeyah et al. (2015) The TMPRSS2-ERG Gene Fusion Blocks XRCC4-Mediated Nonhomologous End-Joining Repair and Radiosensitizes Prostate Cancer Cells to PARP Inhibition. Mol Cancer Ther 14:1896-906
Al-Harbi, Sayer; Choudhary, Gaurav S; Ebron, Jey Sabith et al. (2015) miR-377-dependent BCL-xL regulation drives chemotherapeutic resistance in B-cell lymphoid malignancies. Mol Cancer 14:185
Choudhary, Gaurav S; Tat, Trinh T; Misra, Saurav et al. (2015) Cyclin E/Cdk2-dependent phosphorylation of Mcl-1 determines its stability and cellular sensitivity to BH3 mimetics. Oncotarget 6:16912-25
Babcook, M A; Sramkoski, R M; Fujioka, H et al. (2014) Combination simvastatin and metformin induces G1-phase cell cycle arrest and Ripk1- and Ripk3-dependent necrosis in C4-2B osseous metastatic castration-resistant prostate cancer cells. Cell Death Dis 5:e1536
Stancu, Andreea Lucia; Smith, Mitchell R; Almasan, Alexandru (2014) New agents for the treatment of lymphoid leukemia and lymphoma: focus on recent FDA approvals. Discoveries (Craiova) 2:

Showing the most recent 10 out of 29 publications