A continuous challenge for both single cells and multicellular organisms is that the availability of nutrients is fluctuating constantly. This is particularly the case for cancer cells in solid tumors or exposed to different stromal environments. Hence, cells must sense the amount of nutrients in the environment to coordinate energy-consuming anabolic reactions with energy-producing catabolic reactions. This task is largely carried out by mTOR complex 1 (mTORC1), a protein kinase complex that senses various environmental cues and coordinates anabolic and catabolic processes to regulate cellular homeostasis. mTORC1 is activated only when amino acids, energy sources, oxygen and growth factor levels are sufficient. Under these conditions mTORC1 promotes cell growth by boosting protein, lipid and nucleotide synthesis. However, whereas many of the key players involved in growth factor signaling to mTORC1 have been characterized, much less is understood about how mTORC1 senses amino acids. It is also unclear how different cancer cell-associated mutations provide tumor cells with the ability to optimize usage of these regulatory components or find ways to overcome deficiencies in these mTORC1 regulators. Additionally, once activated it is still a mystery how mTORC1 regulates and coordinates the many processes required to promote cell growth, proliferation, migration, and survival, and how the altered signaling in cancer cells leads to resistance to current mTORC1 therapies with rapamycin (an FDA approved mTORC1 inhibitor). Along these lines it remains unclear how mTORC1 can regulate the variety of biological processes associated with cancer. To better understand mTORC1 signaling, we can now combine our mTORC1 RNAi screens, and phosphoproteome, interactome, metabolome and gene expression data sets, to support our efforts. In this proposal we have outlined several goals based on this new information, our published work and the extensive experience of my lab, that support our long-term goals of defining mTORC1 regulation and signaling, and for revealing new insight to support efforts to kill cancer cells with activated mTORC1 signaling. Our scientific discoveries and experience have now led us to investigate a novel mechanism for responding to amino acid availability (aim 1), a new pathway for regulating nuclear GSK3 signaling and gene expression of targets linked to biological processes hijacked by cancer cells (aims 2 & 3), and novel mechanisms associated with mRNA biogenesis as a means of changing gene expression and increasing protein diversity (aim 4). In conclusion, there's a critical need for a greater understanding of the molecular basis of mTORC1 regulation and signaling, and its links to processes associated with cell growth, migration/invasion, survival and drug resistance. Our expectations are that successful completion of the proposed work will impact cancer biology/physiology and therapy through the identification of new therapeutic targets and biomarkers that will improve detection and elimination of cancer cells with unregulated mTORC1 signaling, estimated to occur in 70-80% of human cancers.

Public Health Relevance

Using our extensive expertise in mTOR signaling and cancer biology, we will establish a new level of understanding of how mTOR is regulated by amino acids and how mTOR in turn regulates several protein kinases and transcription factors involved in gene expression and mRNA biogenesis; areas of mTOR signaling that are critical to mTOR biology but also areas which have received less attention than the currently understood connections between growth factors, mTOR and regulation of protein synthesis, autophagy, and some aspects of metabolism. With the described aims, we will established a novel link between amino acid availability and an intimate Yin-Yang relationship between the GTPases Rap1, and Rag and Rheb; we will characterize a novel connection between mTOR, and previously uncharacterized protein kinase effectors, transcriptional regulators and modulators of metabolism and other mTOR-associated biologies; and finally we will investigate a previously unstudied connection between mTOR and mRNA biogenesis. Our preliminary data place us in the unique position to uncover and understand at a biochemical and molecular level new regulatory processes, new biomarkers and new potential targets for drug discovery that are needed for personalized therapeutic intervention in metabolic diseases such as cancer that are driven by improper mTOR signaling.

Agency
National Institute of Health (NIH)
Institute
National Institute of General Medical Sciences (NIGMS)
Type
Research Project (R01)
Project #
5R01GM051405-24
Application #
9537564
Study Section
Molecular and Integrative Signal Transduction Study Section (MIST)
Program Officer
Marino, Pamela
Project Start
1995-09-01
Project End
2020-07-31
Budget Start
2018-08-01
Budget End
2019-07-31
Support Year
24
Fiscal Year
2018
Total Cost
Indirect Cost
Name
Weill Medical College of Cornell University
Department
Pharmacology
Type
Schools of Medicine
DUNS #
060217502
City
New York
State
NY
Country
United States
Zip Code
10065
He, Long; Gomes, Ana P; Wang, Xin et al. (2018) mTORC1 Promotes Metabolic Reprogramming by the Suppression of GSK3-Dependent Foxk1 Phosphorylation. Mol Cell 70:949-960.e4
Schild, Tanya; Low, Vivien; Blenis, John et al. (2018) Unique Metabolic Adaptations Dictate Distal Organ-Specific Metastatic Colonization. Cancer Cell 33:347-354
Lee, Gina; Zheng, Yuxiang; Cho, Sungyun et al. (2017) Post-transcriptional Regulation of De Novo Lipogenesis by mTORC1-S6K1-SRPK2 Signaling. Cell 171:1545-1558.e18
Gomes, Ana P; Schild, Tanya; Blenis, John (2017) Adding Polyamine Metabolism to the mTORC1 Toolkit in Cell Growth and Cancer. Dev Cell 42:112-114
Yoon, Sang-Oh; Shin, Sejeong; Karreth, Florian A et al. (2017) Focal Adhesion- and IGF1R-Dependent Survival and Migratory Pathways Mediate Tumor Resistance to mTORC1/2 Inhibition. Mol Cell 67:512-527.e4
Wada, Shogo; Neinast, Michael; Jang, Cholsoon et al. (2016) The tumor suppressor FLCN mediates an alternate mTOR pathway to regulate browning of adipose tissue. Genes Dev 30:2551-2564
Li, Jing; Shin, Sejeong; Sun, Yang et al. (2016) mTORC1-Driven Tumor Cells Are Highly Sensitive to Therapeutic Targeting by Antagonists of Oxidative Stress. Cancer Res 76:4816-27
Gomes, Ana P; Blenis, John (2015) A nexus for cellular homeostasis: the interplay between metabolic and signal transduction pathways. Curr Opin Biotechnol 34:110-7
Li, Jing; Csibi, Alfredo; Yang, Sun et al. (2015) Synthetic lethality of combined glutaminase and Hsp90 inhibition in mTORC1-driven tumor cells. Proc Natl Acad Sci U S A 112:E21-9
Shin, Sejeong; Buel, Gwen R; Wolgamott, Laura et al. (2015) ERK2 Mediates Metabolic Stress Response to Regulate Cell Fate. Mol Cell 59:382-98

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