Today, lung cancer is the leading cause of death in both men and women in industrialized countries, accounting for an estimated 28% of all cancer deaths in the United States. Non-small cell lung cancers (NSCLC) represent the majority of lung cancers and carry a poor prognosis with a median survival of less than 12 months. Most patients present with unresectable disease and current treatment options of chemotherapy and radiation are palliative at best. Therefore, new strategies are needed in the treatment of NSCLC in order to impact this disease. In this study, we are focusing on NSCLC models for examining distal signaling mechanisms that modulate the chemotherapy sensitivity, generation, and maintenance of NSCLC cells/tumors. Specifically, this grant application focuses on the survival/oncogenic signaling pathways activated by caspase 9b. The expression of caspase 9b is regulated by alternative splicing via the inclusion or exclusion of a four exon cassette (exons 3, 4, 5, and 6). Inclusion of this exon cassette into the mature transcript produces the pro- apoptotic caspase 9 (caspase 9a) while the exclusion produces the anti-apoptotic and survival signaling factor, caspase 9b. Studies from our laboratory have demonstrated that NSCLC tumors present with a dysregulated (e.g. low) ratio of caspase 9/caspase 9b analogous to an anti-apoptotic/chemotherapy resistance phenotype. Subsequent studies by our laboratory demonstrated that the alternative splicing of caspase 9 had important functions in the anchorage-independent growth (AIG) of NSCLC cells, AIG induced by oncogenic mutation in non-transformed human bronchial epithelial cells, and chemotherapy sensitivity (e.g. cisplatinum and paclitaxel). Mechanistically, our laboratory identified an exonic splicing silencer (C9/E3-ESS) in exon 3 that regulates the inclusion of the exon 3, 4, 5, and 6 cassette of caspase 9 pre-mRNA. hnRNP L was shown to associate with this RNA cis-element, repress the inclusion of the exon cassette, and induce caspase 9b expression. Importantly, phosphorylation of hnRNP L on ser52 (observed only in transformed cells) was required for repression of the exon 3,4,5,6 cassette. Lastly, ser52 phosphorylation of hnRNP L was shown as a required mediator of the tumorigenic capacity of NSCLC cells via the alternative splicing of caspase 9. These key mechanisms are specific to transformed cells, translatable to >70% of NSCLCs, and at an extreme distal point in oncogenic pathways. Therefore, these distal mechanisms are plausible and highly desired targets for the development of new anti-cancer therapeutics. The proposed studies will determine the mechanisms and cell signaling pathways regulated by the survival product of caspase 9 RNA splicing, caspase 9b. These studies will also examine naturally occurring tumor suppression pathways (e.g. sphingolipid pathways) that block the production of caspase 9b, and thereby inhibit the growth of NSCLC tumors. Furthermore, we are proposing pre-clinical studies to determine whether the specific targeting of caspase 9b is effective for treating NSCLC by enhancing the effectiveness of current chemotherapeutic agents used in the clinic (e.g. cisplatinum and paclitaxel).

Public Health Relevance

Cancer is the second leading cause of death among US veterans, and lung cancer is associated with the greatest mortality in these patients. Non-small cell lung cancers (NSCLC) represent the majority of lung cancers and carry a poor prognosis with a median survival of less than 12 months. Most patients present with unresectable disease, and current treatment options of chemotherapy and radiation are palliative at best. Our laboratory has identified key mechanisms specific to cancer cells and translatable to >70% of NSCLCs, which are plausible and highly desired targets for the development of new anti-cancer therapeutics. This grant application explores these cellular mechanisms in depth with the goal of developing new therapeutics to combat NSCLC, and thereby, aid US Veterans.

Agency
National Institute of Health (NIH)
Institute
Veterans Affairs (VA)
Type
Non-HHS Research Projects (I01)
Project #
5I01BX001792-04
Application #
8965985
Study Section
Oncology A (ONCA)
Project Start
2012-10-01
Project End
2016-09-30
Budget Start
2015-10-01
Budget End
2016-09-30
Support Year
4
Fiscal Year
2016
Total Cost
Indirect Cost
Name
VA Veterans Administration Hospital
Department
Type
DUNS #
146678115
City
Richmond
State
VA
Country
United States
Zip Code
23249
Karandashova, Sophia; Kummarapurugu, Apparao B; Zheng, Shuo et al. (2018) Neutrophil elastase increases airway ceramide levels via upregulation of serine palmitoyltransferase. Am J Physiol Lung Cell Mol Physiol 314:L206-L214
Mishra, Shrawan Kumar; Gao, Yong-Guang; Deng, Yibin et al. (2018) CPTP: A sphingolipid transfer protein that regulates autophagy and inflammasome activation. Autophagy 14:862-879
Vhuiyan, Mynol I; Pak, Magnolia L; Park, Margaret A et al. (2017) PRMT2 interacts with splicing factors and regulates the alternative splicing of BCL-X. J Biochem 162:17-25
Contaifer Jr, Daniel; Carl, Daniel E; Warncke, Urszula Osinska et al. (2017) Unsupervised analysis of combined lipid and coagulation data reveals coagulopathy subtypes among dialysis patients. J Lipid Res 58:586-599
DeLigio, James T; Lin, Grace; Chalfant, Charles E et al. (2017) Splice variants of cytosolic polyadenylation element-binding protein 2 (CPEB2) differentially regulate pathways linked to cancer metastasis. J Biol Chem 292:17909-17918
Stephenson, Daniel J; Hoeferlin, L Alexis; Chalfant, Charles E (2017) Lipidomics in translational research and the clinical significance of lipid-based biomarkers. Transl Res 189:13-29
Qi, Hui; Priyadarsini, Shrestha; Nicholas, Sarah E et al. (2017) Analysis of sphingolipids in human corneal fibroblasts from normal and keratoconus patients. J Lipid Res 58:636-648
Priyadarsini, Shrestha; McKay, Tina B; Sarker-Nag, Akhee et al. (2016) Complete metabolome and lipidome analysis reveals novel biomarkers in the human diabetic corneal stroma. Exp Eye Res 153:90-100
Truchan, Hilary K; VieBrock, Lauren; Cockburn, Chelsea L et al. (2016) Anaplasma phagocytophilum Rab10-dependent parasitism of the trans-Golgi network is critical for completion of the infection cycle. Cell Microbiol 18:260-81
Vu, Ngoc T; Park, Margaret A; Shultz, Michael D et al. (2016) Caspase-9b Interacts Directly with cIAP1 to Drive Agonist-Independent Activation of NF-?B and Lung Tumorigenesis. Cancer Res 76:2977-89

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