Abstract

Rapamycins are novel anticancer agents that specifically inhibit the activity of a protein Ser/Thr kinase (mTOR) that controls translation of proteins involved in cell cycle progression and survival. At present two analogues, CCI-779 and RAD001, are in clinical development, and have shown antitumor activity in phase I and II trials. In the last period of funding our studies demonstrated that rapamycin induces apoptosis only in cells lacking a functional p53/p21Cip1 pathway. This, therefore, presents a biochemical rationale for tumor-selective killing. Rapamycin-induced apoptosis is a consequence of mTOR inhibition that rapidly induces cellular stress, characterized by activation of apoptosis signaling kinase 1 (ASK1). This leads to activation of Jun N-terminal kinase, and increased levels of phospho-c-Jun. Of importance is the observation that this stress response is rapidly suppressed in cells with functional p53 in a p21Cip1 dependent manner. However, suppression of apoptosis is not a consequence of p53/p21Cip1mediated cell cycle arrest. Rather, rapamycin treatment leads to the association of ASK1 with p21Cip1 and suppression of ASK1 activity. Preliminary results demonstrate that amino acid deprivation mimics the rapamycin-induced stress response. In this application we propose a series of studies that will determine: 1. Whether the rapamycin-induced stress response is a consequence of inhibition of mTOR kinase function, and results from inhibition of signaling to 4E-BP, S6K1 or protein phosphatase 5 (PP5). 2. How rapamycin treatment induces binding of p21Cip1 to ASK1, and determine whether activation of Jun N-terminal kinase (JNK) or elevated P-c-Jun is required for complex formation. 3. Domains of p21Cip1 and ASK1 required for complex formation. 4. Whether the cellular stress induced by amino acid deprivation is similar to that induced by rapamycin, and determine whether the p53/p21 axis is required to suppress nutritional stress. We propose that the rapamycin-induced stress response is a fundamental response to mTOR inhibition, and that p53/p21Cip1 function is essential to protect cells from apoptosis in nutritionally deficient environments. The work proposed in this application will help elucidate the synthetic lethal interaction that is induced by rapamycins only in cells with mutations that predispose to cancer formation, i.e. p53 or p21Cip1. Our studies will develop the biochemical framework to underpin a novel approach by which rapamycins can induce tumor-selective cytotoxicity based on the loss of the tumor suppressor p53.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Research Project (R01)
Project #
5R01CA077776-07
Application #
6913562
Study Section
Experimental Therapeutics Subcommittee 1 (ET)
Program Officer
Forry, Suzanne L
Project Start
1998-12-01
Project End
2008-04-30
Budget Start
2005-07-01
Budget End
2006-04-30
Support Year
7
Fiscal Year
2005
Total Cost
$282,000
Indirect Cost

  Institution

Name
St. Jude Children's Research Hospital
Department
Type
DUNS #
067717892
City
Memphis
State
TN
Country
United States
Zip Code
38105

  Publications

Zhou, Xinhui; Liu, Weijin; Hu, Xing et al. (2017) Regulation of CHK1 by mTOR contributes to the evasion of DNA damage barrier of cancer cells. Sci Rep 7:1535
He, Zhengfu; Hu, Xing; Liu, Weijin et al. (2017) P53 suppresses ribonucleotide reductase via inhibiting mTORC1. Oncotarget 8:41422-41431
Phelps, Doris; Bondra, Kathryn; Seum, Star et al. (2015) Inhibition of MDM2 by RG7388 confers hypersensitivity to X-radiation in xenograft models of childhood sarcoma. Pediatr Blood Cancer 62:1345-52
Studebaker, Adam; Bondra, Kathryn; Seum, Star et al. (2015) Inhibition of MEK confers hypersensitivity to X-radiation in the context of BRAF mutation in a model of childhood astrocytoma. Pediatr Blood Cancer 62:1768-74
Woods, Gary M; Bondra, Kathryn; Chronowski, Christopher et al. (2015) Radiation therapy may increase metastatic potential in alveolar rhabdomyosarcoma. Pediatr Blood Cancer 62:1550-1554
Adamson, Peter C; Houghton, Peter J; Perilongo, Giorgio et al. (2014) Drug discovery in paediatric oncology: roadblocks to progress. Nat Rev Clin Oncol 11:732-9
Cam, Maren; Bid, Hemant K; Xiao, Linlin et al. (2014) p53/TAp63 and AKT regulate mammalian target of rapamycin complex 1 (mTORC1) signaling through two independent parallel pathways in the presence of DNA damage. J Biol Chem 289:4083-94
Singh, Mamata; Leasure, Justin M; Chronowski, Christopher et al. (2014) FANCD2 is a potential therapeutic target and biomarker in alveolar rhabdomyosarcoma harboring the PAX3-FOXO1 fusion gene. Clin Cancer Res 20:3884-95
Shen, Changxian; Oswald, Duane; Phelps, Doris et al. (2013) Regulation of FANCD2 by the mTOR pathway contributes to the resistance of cancer cells to DNA double-strand breaks. Cancer Res 73:3393-401
Shen, Changxian; Houghton, Peter J (2013) The mTOR pathway negatively controls ATM by up-regulating miRNAs. Proc Natl Acad Sci U S A 110:11869-74

Showing the most recent 10 out of 48 publications