Abstract

The overall goal of this project is to expand our understanding of the cellular and molecular mechanisms that link translation initiation inhibition to apoptosis and tumor suppression triggered by Interleukin-24 (IL-24). Clinical testing of IL-24 as a gene-based therapeutic for the treatment of solid tumors demonstrated that IL-24 is efficacious and is safe. This proposal is consistent with the current view that modern anti-cancer therapy must be target-specific, inhibit the growth of cancer with minimal effect on normal cells, and that effective anti- cancer agents of low toxicity can be achieved by targeting the fundamental mechanisms responsible for the genesis, maintenance, and/or progression of cancer. I have shown that IL-24 causes partial depletion of intracellular Ca++ and activation of endoplasmic reticulum (ER) stress, which in turn induces inhibitory phosphorylation of eukaryotic initiation factor 2 alpha (eIF2?). Phosphorylation of eIF2? and the availability of he ternary complex control not only the overall rate of translation, as initially thought, but also th expression of specific gene clusters. The tight translational control of most oncogenic proteins explains the link between unrestricted translation initiation and malignant transformation that has been well established in both experimental models and in numerous human cancers that overexpress translation initiation factors. Phosphorylated eIF2? binds with high affinity to the guanine nucleotide exchange factor eIF2B and thereby inhibits recycling of eIF2*GDP into eIF2*GTP, depleting the ternary complex necessary to initiate a new round of translation. It is well established that partial depletion of ER Ca++ stores activates the eIF2? kinases that phosphorylate eIF2? and thereby limits the rate of translation initiation. Furthermore, I have demonstrated that IL-24 induces expression of Binding immunoglobulin protein (BiP) and C/-EBP homologous protein (CHOP), two down-stream markers of ternary complex abundance. The working hypothesis of this application is that IL-24 exerts anticancer activities because it helps restore physiological restraints on translation initiation. I have demonstrated that Sigma 1 Receptor (Sig1R) interacts with IL-24 and that this IL-24:Sig1R is a critical upstream signal for IL-24-induced ER-stress, calcium mobilization, phosphorylation of eIF2? and apoptosis on cancer cells. In this application we propose to continue our efforts to characterize the cancer cell- specific actions of IL-24 as an inhibitor of translation initiation. Specifically, we will 1)use cameleon calcium indicator proteins to assess directly the calcium content of the ER-stores after IL-24 treatment (Specific Aim 1), 2) determine whether depletion of the ternary complex mediates the anticancer effect of IL-24, (Specific Aim 2), and 3) determine the role of Sig1R on IL-24-mediated inhibition of translation initiation (Specific Aim 3). For these proposed studies we will collaborate with Dr. Jose A. Halperin, from Harvard Medical School, and expert on targeting translation initiation for cancer therapy.

Public Health Relevance

Cancer ranks as the second leading cause of death in men and women of all age groups in the U.S., and currently 1 out of 4 deaths in the U.S. is due to cancer. The severe adverse effects due to many anti-cancer therapeutic strategies currently in use are associated with their undesired effects on healthy, non-cancer cells. This project, therefore, is directed toward understanding cellular and molecular mechanisms that will help develop a specific cancer therapy that only kills tumor cells. To this end, we will investigate the role of translation initiation inhibition in the tumor suppression triggered by an anti-cancer agen, Interleukin 24. The ultimate goal is to identify novel therapeutic targets for treating cancer.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Research Enhancement Award (SC1)
Project #
5SC1CA200518-03
Application #
9319703
Study Section
Special Emphasis Panel (ZGM1)
Program Officer
Chung, Davyd W
Project Start
2015-08-01
Project End
2019-07-31
Budget Start
2017-08-01
Budget End
2018-07-31
Support Year
3
Fiscal Year
2017
Total Cost
Indirect Cost

  Institution

Name
Herbert H. Lehman College
Department
Biology
Type
Schools of Arts and Sciences
DUNS #
620128301
City
New York
State
NY
Country
United States
Zip Code
10468

  Publications

Kasteri, Justina; Das, Dibash; Zhong, Xuelin et al. (2018) Translation Control by p53. Cancers (Basel) 10:
Zhong, Xuelin; Persaud, Leah; Muharam, Hilal et al. (2018) Eukaryotic Translation Initiation Factor 4A Down-Regulation Mediates Interleukin-24-Induced Apoptosis through Inhibition of Translation. Cancers (Basel) 10:
Persaud, Leah; Zhong, Xuelin; Alvarado, Giselle et al. (2017) eIF2? Phosphorylation Mediates IL24-Induced Apoptosis through Inhibition of Translation. Mol Cancer Res 15:1117-1124
Persaud, Leah; De Jesus, Dayenny; Brannigan, Oliver et al. (2016) Mechanism of Action and Applications of Interleukin 24 in Immunotherapy. Int J Mol Sci 17: