Abstract

The transcription factor nuclear factor kappaB (NF-kappaB) has been linked to acquired therapeutic resistance in multiple types of human cancer by inhibiting cell death and drug sensitivity of malignant cells. Various genotoxic agents used in cancer treatment, such as chemotherapeutic drugs and irradiation, have been shown to activate NF-kappaB, which is a major impediment to effective cancer treatment. Our long term goal is to improve efficacy of radio/chemotherapy and reduce the resistance of cancer cells by modulating the genotoxic NF-kappaB signaling pathway. Our previous studies established a conserved nuclear-to-cytoplasmic signaling pathway which orchestrates NF-kappaB activation induced by a broad range of genotoxic therapeutic agents. We found ELKS (a protein rich in glutamate, leucine, lysine and serine) is indispensable for the activation of IKK complex and NF-kappaB by genotoxic agents. Our preliminary studies indicate posttranslational modifications of ELKS, such as ubiquitination and phosphorylation, orchestrate the process of ATM-dependent IKK activation, resulting in NF-kappaB activation in response to genotoxic therapeutic agents. Genetic ablation of ELKS significantly increases the mortality in mice exposed to ionized radiation. We hypothesize that DNA damage-induced ELKS posttranslational modifications play critical roles in genotoxic NF-kappaB signaling pathway, and modulating genotoxic NF-kappaB activation may sensitize tumor cells to genotoxic agent-induced cell death. We will test the hypothesis with the following specific aims:
Aim 1 is to characterize the ubiquitination of ELKS in genotoxic NF-kappaB signaling pathway.
In aim 2, we will delineate how ATM regulates ELKS ubiquitination induced by genotoxic stress. We will further determine biological functions of ELKS mediated DNA damage response and its impact on therapeutic resistance in vivo in Aim3. Completion of the proposed specific aims outlined in this grant proposal will advance our understanding of the molecular mechanism governing the ELKS-mediated genotoxic NF- kappaB signaling and its function in regulating therapeutic resistance. Furthermore, the exploration of the non-neuronal function of ELKS and potential cytoplasmic activity of ATM may reveal novel research paradigm which may greatly broaden our knowledge in the physiological and pathological functions of these important molecules. We envision the selective inhibition of NF-kappaB activity by targeting specific signaling mechanisms will effectively alleviate the therapeutic resistance while keeping immune response intact in cancer patients.

Public Health Relevance

One of the major obstacles to effective cancer treatment is the development of therapeutic resistance by cancer cells, which may lead to recurrence of the cancer or even death of the patient. By elucidating molecular mechanisms and biological functions of the signaling pathways helping cancer cells evade from demise induced by tumor therapeutic agents, the present studies will provide insights into how these agents induce therapeutic resistance in malignant cells, which will lead to novel strategies for improving the efficacy of cancer treatment through sensitizing tumor cells to chemotherapy and irradiation.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Research Project (R01)
Project #
5R01CA149251-05
Application #
8790742
Study Section
Basic Mechanisms of Cancer Therapeutics Study Section (BMCT)
Program Officer
Arya, Suresh
Project Start
2011-01-01
Project End
2015-12-31
Budget Start
2015-01-01
Budget End
2015-12-31
Support Year
5
Fiscal Year
2015
Total Cost
$307,100
Indirect Cost
$99,600

  Institution

Name
University of Tennessee Health Science Center
Department
Pathology
Type
Schools of Medicine
DUNS #
941884009
City
Memphis
State
TN
Country
United States
Zip Code
38103

  Publications

Huang, Sheng; Chi, Yayun; Qin, Yi et al. (2018) CAPG enhances breast cancer metastasis by competing with PRMT5 to modulate STC-1 transcription. Theranostics 8:2549-2564
Chen, Hongfeng; Sirupangi, Tirupataiah; Wu, Zhao-Hui et al. (2018) The conserved RNA recognition motif and C3H1 domain of the Not4 ubiquitin ligase regulate in vivo ligase function. Sci Rep 8:8163
Wang, Wei; Zhang, Bo; Mani, Arul M et al. (2018) Survivin Inhibitors Mitigate Chemotherapeutic Resistance in Breast Cancer Cells by Suppressing Genotoxic Nuclear Factor-?B Activation. J Pharmacol Exp Ther 366:184-193
Pop-Bica, Cecilia; Pintea, Sebastian; Cojocneanu-Petric, Roxana et al. (2018) MiR-181 family-specific behavior in different cancers: a meta-analysis view. Cancer Metastasis Rev 37:17-32
Wang, Wei; Mani, Arul M; Wu, Zhao-Hui (2017) DNA damage-induced nuclear factor-kappa B activation and its roles in cancer progression. J Cancer Metastasis Treat 3:45-59
Sethuraman, Aarti; Brown, Martin; Seagroves, Tiffany N et al. (2016) SMARCE1 regulates metastatic potential of breast cancer cells through the HIF1A/PTK2 pathway. Breast Cancer Res 18:81
Xue, J; Chi, Y; Chen, Y et al. (2016) MiRNA-621 sensitizes breast cancer to chemotherapy by suppressing FBXO11 and enhancing p53 activity. Oncogene 35:448-58
Wu, Zhao-Hui; Pfeffer, Lawrence M (2016) MicroRNA regulation of F-box proteins and its role in cancer. Semin Cancer Biol 36:80-7
Niu, Jixiao; Xue, Aimin; Chi, Yayun et al. (2016) Induction of miRNA-181a by genotoxic treatments promotes chemotherapeutic resistance and metastasis in breast cancer. Oncogene 35:1302-1313
Wang, Wei; Huang, Xuan; Xin, Hong-Bo et al. (2015) TRAF Family Member-associated NF-?B Activator (TANK) Inhibits Genotoxic Nuclear Factor ?B Activation by Facilitating Deubiquitinase USP10-dependent Deubiquitination of TRAF6 Ligase. J Biol Chem 290:13372-85

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