Abstract

A p53/NFkB-mediated metabolic mechanism for chemotherapy protection Chemotherapy remains the current front line cancer treatment, but the resulting severe side effects often pose a significant threat to cancer patients, raising a pressin need for the development of effective strategies for chemotherapy protection. We found that low-dose arsenic pretreatment markedly alleviates the chemotherapy toxicity, and that arsenic does so via induction of glycolysis. Of significance is that arsenic-mediated protection absolutely requires functional p53, making it possible to selectively protect only normal tissues but not cancer cells. Using tumor xenograft mouse models, we demonstrated the effectiveness of this approach. We hypothesize that the p53-mediated metabolic reprogramming is a novel mechanism of chemotherapy protection. We'll test the hypothesis by; 1) directly linking glycolysis and glycolytic enzymes to chemotherapy protection; 2) exploring the mechanisms responsible for metabolic regulation of cellular sensitivity to chemotherapy, 3) investigating p53-mediated metabolic regulation of hematopoietic stem cells (HSC). When successfully completed, the proposed studies would uncover a novel metabolic strategy for chemotherapy protection. Significance: Chemotherapy kill cancer cells primarily via induction of DNA damage, which also affects normal tissues by strongly activating p53 causing pathological consequences. We have exploited low-dose arsenic-induced transient p53 inhibition to selectively reduce chemotherapeutics toxicity in normal tissues. Our recent studies with tumor-bearing mice have provided proof-of-principle for the proposed approach. The proposed investigation into the p53/NFkB/HIF-1a axis- mediated metabolic regulation of cell and tissue sensitivity to chemotherapy may yield a new mechanism of normal tissue protection, which would enable the development of novel strategies to alleviate chemotherapy toxicity. We have a proven record in the proposed areas of cancer research and are uniquely positioned to carry out the outlined studies. The overarching goal of this research is to provide more effective treatment for cancer patients by minimizing adverse side effects and thereby to reduce patient mortality and to improve quality of life. The proposed work has potential to impact cancer patient care in a fundamental way. Innovation: The innovative nature of this proposal lies in the focus of our study on the metabolic mechanism of chemotherapy protection. Our preliminary studies have established several in vitro and in vivo metabolic markers and assays, which are exquisitely sensitive and should enable us to investigate mechanisms by which metabolic pathways regulate cellular and tissue sensitivity to chemotherapy. The absolute requirement of functional p53 and its antagonistic interaction with NFkB/HIF-1a in low-dose arsenic-mediated defense provides a sound foundation for selective protection to normal tissues. The metabolic regulation of chromatin modification represents a novel mechanism of chemotherapy protection. The glycolysis-mediated fitness and stress tolerance of HSCs may offer a new method of protecting HSCs from chemotherapy toxicity.

Public Health Relevance

The overarching goal of this research is to provide more effective treatment for cancer patients by minimizing adverse side effects and thereby to reduce patient mortality and to improve quality of life. The proposed work has potential to impact patient care in a fundamental way.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Research Project (R01)
Project #
5R01CA183074-05
Application #
9461950
Study Section
Basic Mechanisms of Cancer Therapeutics Study Section (BMCT)
Program Officer
Arya, Suresh
Project Start
2014-04-01
Project End
2019-03-31
Budget Start
2018-04-01
Budget End
2019-03-31
Support Year
5
Fiscal Year
2018
Total Cost
Indirect Cost

  Institution

Name
Harvard University
Department
Genetics
Type
Schools of Public Health
DUNS #
149617367
City
Boston
State
MA
Country
United States
Zip Code

  Publications

de Polo, Anna; Luo, Zhongling; Gerarduzzi, Casimiro et al. (2017) AXL receptor signalling suppresses p53 in melanoma through stabilization of the MDMX-MDM2 complex. J Mol Cell Biol 9:154-165
Yang, M; Lewinska, M; Fan, X et al. (2016) PRR14 is a novel activator of the PI3K pathway promoting lung carcinogenesis. Oncogene 35:5527-5538
Gong, Lu; Pan, Xiao; Yuan, Zhi-Min et al. (2016) p53 coordinates with ?133p53 isoform to promote cell survival under low-level oxidative stress. J Mol Cell Biol 8:88-90
Ha, Chul S; Michalek, Joel E; Elledge, Richard et al. (2016) p53-based strategy to reduce hematological toxicity of chemotherapy: A proof of principle study. Mol Oncol 10:148-56
de Polo, Anna; Vivekanandan, Varunika; Little, John B et al. (2016) MDMX under stress: the MDMX-MDM2 complex as stress signals hub. Transl Cancer Res 5:725-732
Liu, X-S; Liu, Z; Gerarduzzi, C et al. (2016) Somatic human ZBTB7A zinc finger mutations promote cancer progression. Oncogene 35:3071-8
Qi, Min; Ganapathy, Suthakar; Zeng, Weiqi et al. (2015) UXT, a novel MDMX-binding protein, promotes glycolysis by mitigating p53-mediated restriction of NF-?B activity. Oncotarget 6:17584-93
Liu, Xue-Song; Little, John B; Yuan, Zhi-Min (2015) Glycolytic metabolism influences global chromatin structure. Oncotarget 6:4214-25
Su, Hang; Ganapathy, Suthakar; Li, Xiaolei et al. (2015) p53-Based Strategy for Protection of Bone Marrow From Y-90 Ibritumomab Tiuxetan. Int J Radiat Oncol Biol Phys 92:1116-1122
Lall, R; Ganapathy, S; Yang, M et al. (2014) Low-dose radiation exposure induces a HIF-1-mediated adaptive and protective metabolic response. Cell Death Differ 21:836-44

Showing the most recent 10 out of 11 publications