Abstract

Metabolic imaging using hyperpolarized (HP) 13C and 15N substrates offers the potential to monitor intermediary metabolism in tissues throughout the human body. HP-[1-13C]pyruvate is the molecule most widely used in HP studies, but there are several other TCA cycle intermediates that meet the requirements of a good metabolic imaging candidate probe. In this TR&D Project we propose to develop new 13C- and 15N-enriched compounds as reporters of tissue physiology and metabolism. We will apply these hyperpolarized sensors to measure important physiological parameters at sensitivity levels never before achieved by MRI. One of the main thrusts of this proposal is to develop HP-13C labeled mono-esters of TCA cycle intermediates to image whole-body glucose production because this could potentially have an enormous impact on development of new drugs to control glucose levels in type 2 diabetic patient populations. Thus, Aim 1 will focus on the design, synthesis and DNP hyperpolarization of monoesters of 13C-labeled TCA cycle intermediates such as [4-13C]oxaloacetate-1-ethyl ester, [4-13C]malate-1-ethyl ester, and [1-13C]-2-ketoglutarate-4-ethyl ester. The 13C-enriched carbon in these molecules should display long T1 values and these derivatives should enter hepatocytes quickly via mono-carboxylate transporters and hydrolyze to their respective dicarboxylate intermediates. 15N is another attractive nucleus for the design of HP-probes but its potential for metabolic imaging has largely remained unexplored.
In Aim 2 novel 15N- labeled molecular design platforms are proposed that will yield HP-15N-agents for imaging pH and free Zn2+-levels in zinc-rich tissues.. Considering the fact that HP-[1-13C]pyruvate is the most popular molecule of choice for metabolic MR imaging, in Aim 3, a practical chemical approach will be developed to produce gram quantities of HP-[1-13C]pyruvate by starting with an ester of pyruvate and para-H2. If we are successful, this would make HP-[1-13C]pyruvate more widely available to MRI clinics across the country for molecular imaging of cancer and other metabolic diseases. The overarching goal of this core project is to develop and implement novel hyperpolarized agents in vivo to image important biomarkers and metabolic pathways in type 2 diabetes, cancer and other diseases.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Biomedical Imaging and Bioengineering (NIBIB)
Type
Biotechnology Resource Grants (P41)
Project #
2P41EB015908-29
Application #
9209325
Study Section
Special Emphasis Panel (ZEB1)
Project Start
1997-09-01
Project End
2021-12-31
Budget Start
2016-09-01
Budget End
2017-08-31
Support Year
29
Fiscal Year
2017
Total Cost
Indirect Cost

  Institution

Name
University of Texas Sw Medical Center Dallas
Department
Type
DUNS #
800771545
City
Dallas
State
TX
Country
United States
Zip Code
75390

  Publications

Wu, Cheng-Yang; Satapati, Santhosh; Gui, Wenjun et al. (2018) A novel inhibitor of pyruvate dehydrogenase kinase stimulates myocardial carbohydrate oxidation in diet-induced obesity. J Biol Chem 293:9604-9613
Ren, Jimin; Shang, Ty; Sherry, A Dean et al. (2018) Unveiling a hidden 31 P signal coresonating with extracellular inorganic phosphate by outer-volume-suppression and localized 31 P MRS in the human brain at 7T. Magn Reson Med 80:1289-1297
Burnett, Marianne E; Adebesin, Bukola; Ratnakar, S James et al. (2018) Crystallographic Characterization and Non-Innocent Redox Activity of the Glycine Modified DOTA Scaffold and Its Impact on EuIII Electrochemistry. Eur J Inorg Chem 2018:1556-1562
Cui, Jiaming; Dimitrov, Ivan E; Cheshkov, Sergey et al. (2018) An Adjustable-Length Dipole Using Forced-Current Excitation for 7T MR. IEEE Trans Biomed Eng 65:2259-2266
Sirusi, Ali A; Suh, Eul Hyun; Kovacs, Zoltan et al. (2018) The effect of Ho3+ doping on 13C dynamic nuclear polarization at 5 T. Phys Chem Chem Phys 20:728-731
Courtney, Kevin D; Bezwada, Divya; Mashimo, Tomoyuki et al. (2018) Isotope Tracing of Human Clear Cell Renal Cell Carcinomas Demonstrates Suppressed Glucose Oxidation In Vivo. Cell Metab 28:793-800.e2
Potts, Austin; Uchida, Aki; Deja, Stanislaw et al. (2018) Cytosolic phosphoenolpyruvate carboxykinase as a cataplerotic pathway in the small intestine. Am J Physiol Gastrointest Liver Physiol 315:G249-G258
Wu, Cheng-Yang; Tso, Shih-Chia; Chuang, Jacinta L et al. (2018) Targeting hepatic pyruvate dehydrogenase kinases restores insulin signaling and mitigates ChREBP-mediated lipogenesis in diet-induced obese mice. Mol Metab 12:12-24
Jin, Eunsook S; Browning, Jeffrey D; Murphy, Rebecca E et al. (2018) Fatty liver disrupts glycerol metabolism in gluconeogenic and lipogenic pathways in humans. J Lipid Res 59:1685-1694
Makarewich, Catherine A; Baskin, Kedryn K; Munir, Amir Z et al. (2018) MOXI Is a Mitochondrial Micropeptide That Enhances Fatty Acid ?-Oxidation. Cell Rep 23:3701-3709

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