Abstract #3027

Towards Imaging the Glycolytic and Glutaminolytic Differences in Prostate Cancer Cell Lines that Affects Outcome of Glutaminase Inhibition

Niki Zacharias Millward ^1,2, Christopher McCullough³, Sriram Shanmugavelandy¹, Jaehyuk Lee¹, Youngbok Lee⁴, James McHenry⁵, Lawrence Jones ⁶, and Pratip Bhattacharya⁷

¹Cancer Systems Imaging, MD Anderson Cancer Center, Houston, TX, United States, ²Bioengineering, Rice University, Houston, TX, United States, ³Institute for Bioscience and Biotechnology Research, National Institute of Standards and Technology, Rockville, MD, United States, ⁴Applied Chemistry, Hanyang University, Korea, Republic of, ⁵University of Houston Downtown Campus, Houston, TX, ⁶Huntington Medical Research Institutes, Pasadena, CA, ⁷MD Anderson Cancer Center, Houston, TX, United States

To understand and image how metabolism changes in prostate cancer (PCa), we determined both extracellular and intracellular metabolic profile of four PCa cell lines with varying degrees of aggressiveness. Differences in metabolism and mechanistic link were further explored using carbon-13 glucose and glutamine feeding studies and hyperpolarized pyruvate metabolic imaging trials with subcutaneous xenograft PC3 and PC3M animal models. We found increased glutamine utilization in the more metastatic cell line PC3M and this increased dependence on glutamine leads to reduction in cell proliferation and ATP when cells are treated with glutaminase inhibitor CB-839. No reduction is seen in PC3 line.

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