Cancers are diseases of uncontrolled cell growth in which cells acquire mutations that lead to cell proliferation outside of the context of normal tissue development. Molecular advances over the past 30 years have characterized many of the signal transduction pathways and gene transcription networks that are altered during cancer progression. Aberrant regulation of these networks invariably results in gross alterations of the metabolic network. Differences in the metabolism of glucose in tumors compared to that of normal tissue have been noted for over 70 years; yet, the origins, consequences, cancer specificities, and the principles of intervention are poorly understood. Our understanding of cancer cell metabolism is challenged by the enormous complexity of the interaction between metabolic pathways and the genetic aberrations that alter these pathways. Advances will require new technologies and conceptual frameworks, such as high-throughput metabolomics, a technique that aims to quantify within a single measurement, a large number of small-molecules within cells and tissues, and mathematical models that can parse the effects of many simultaneous interactions. Investing such effort has the potential to fundamentally alter our understanding of basic cancer biology and lead to innovative therapies. My proposed research focuses on this central problem of cancer cell growth and development and utilizes the application of computational methods rooted in systems biology in conjunction with the use high-throughput technologies such as mass spectrometry-based metabolomics to understand mechanisms that lead to unregulated growth and altered metabolism in cancer cells and primary tumors. During my postdoctoral work, I discovered two novel metabolic pathways in cells undergoing rapid proliferation and tumor development. These studies combined metabolomics technology with techniques I acquired in my postdoctoral training involving cell biology, biochemistry and genetics. One pathway involves an alternate route of glucose uptake that decouple catabolic glucose metabolism with energy metabolism. The other involves the diversion of glycolytic flux into anabolic metabolism through a glycolytic intermediate. Further genetic studies established that this pathway is selected for in the development of human cancer. I will continue these projects during the remainder of my postdoctoral training in the mentored phase. This work will allow me to establish an independent research program involving using systems biology techniques to investigate define biological problems in understanding the role of glucose metabolism in cancer. My previous training in systems biology and current training in a leading cancer biology and signal transduction lab provides a skill-set that is uniquely suited to approach this problem.

Public Health Relevance

The goal of this proposal is to employ a multidisciplinary approach to understanding and intervening in human cancer. Cancer is the leading source of human mortality in the developed world. Cancer cells have different nutritional requirements from that of their normal counterparts and this proposal aims to further understand of the nature of this altered metabolism.

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Research Transition Award (R00)
Project #
7R00CA168997-04
Application #
9168188
Study Section
Subcommittee G - Education (NCI)
Program Officer
Li, Jerry
Project Start
2015-10-17
Project End
2016-02-28
Budget Start
2015-12-18
Budget End
2016-02-28
Support Year
4
Fiscal Year
2015
Total Cost
$234,059
Indirect Cost
$83,053
Name
Duke University
Department
Pharmacology
Type
Schools of Medicine
DUNS #
044387793
City
Durham
State
NC
Country
United States
Zip Code
27705
Dai, Ziwei; Mentch, Samantha J; Gao, Xia et al. (2018) Methionine metabolism influences genomic architecture and gene expression through H3K4me3 peak width. Nat Commun 9:1955
Dai, Ziwei; Locasale, Jason W (2018) Thermodynamic constraints on the regulation of metabolic fluxes. J Biol Chem 293:19725-19739
Hwang, Inah; Oh, Hwanhee; Santo, Evan et al. (2018) FOXO protects against age-progressive axonal degeneration. Aging Cell 17:
Zhao, Fei; Xiao, Christine; Evans, Kathy S et al. (2018) Paracrine Wnt5a-?-Catenin Signaling Triggers a Metabolic Program that Drives Dendritic Cell Tolerization. Immunity 48:147-160.e7
Reid, Michael A; Allen, Annamarie E; Liu, Shiyu et al. (2018) Serine synthesis through PHGDH coordinates nucleotide levels by maintaining central carbon metabolism. Nat Commun 9:5442
Liu, Xiaojing; Cooper, Daniel E; Cluntun, Ahmad A et al. (2018) Acetate Production from Glucose and Coupling to Mitochondrial Metabolism in Mammals. Cell 175:502-513.e13
Gao, Xia; Lee, Katie; Reid, Michael A et al. (2018) Serine Availability Influences Mitochondrial Dynamics and Function through Lipid Metabolism. Cell Rep 22:3507-3520
Mehrmohamadi, Mahya; Jeong, Seong Ho; Locasale, Jason W (2017) Molecular features that predict the response to antimetabolite chemotherapies. Cancer Metab 5:8
Glass, Oliver K; Bowie, Michelle; Fuller, Julie et al. (2017) Differential response to exercise in claudin-low breast cancer. Oncotarget 8:100989-101004
McDonald, Oliver G; Li, Xin; Saunders, Tyler et al. (2017) Epigenomic reprogramming during pancreatic cancer progression links anabolic glucose metabolism to distant metastasis. Nat Genet 49:367-376

Showing the most recent 10 out of 74 publications