Abstract

The ten peer-reviewed and NIH funded Collaborative Projects and the eight Service Projects from leading hyperpolarized MR sites, that are the scientific driving force behind the HMTRC, demonstrate a clear need for the improved HP probes and techniques, realistic pre-clinical models and correlative pathology and biology methodologies that will be provided by this TR&D project. TR&D2 builds on our significant experience in the DNP polarization/dissolution process, the development of new hyperpolarized molecular probe preparations, and in the development and testing of novel biologically relevant NMR-compatible pre-clinical cell/tissue culture and associated novel cell/tissue graft murine models. In the current funding cycle, we developed new 13C labeled HP probes of glycolysis, TCA cycle and cellular redox as well as multi-polarization approaches that provide simultaneous information on metabolism, perfusion, and extracellular pH (pHe). Through this renewal, we aim to greatly improve these HP probes and methods with an emphasis on increased sensitivity, robustness, cost-effectiveness, ease of dissemination, and translatability. This will be accomplished through the use of glassing agents, chemically optimized new radicals, and polarization methods. We will also investigate novel HP probes of pHe, ROS and immune response and to address new questions raised by the CP's (aim 1). In this renewal, we will also investigate new long-lived hyperpolarized probes and use of lower field MRI scanners in order to prolong the T1's of hyperpolarized probes. In the current project, novel 10 and 5 mm MR and PET compatible 3D cell and tissue culture bioreactors were micro-engineered, robustly and cost- effectively produced, and extensively tested and validated in cell and tissue culture studies performed in the CP's. Driven by the needs of the CP's, we now propose future bioreactor designs incorporating new biologic measurement capabilities, addition of novel cell culture constructs, development of a micro-bioreactor system, and extension of human cell & tissue bioreactor studies to novel murine models (aim 2). TR&D2 also made substantial progress developing and implementing procedures to provide correlative pathologic, biologic and imaging data critical for understanding and validating HP MR findings in the CP's. As requested by the EAC and CP's, these validation studies will be augmented by the addition of new metabolomics, enzyme activity staining assays, and PET/HP MR correlative studies (aim 3). While the HP MR probes, model systems and correlative methodologies have been specifically developed for the CP's through a highly productive push-pull approach, these technology developments also have significantly benefited the SP's and the HP MR community in general through extensive dissemination and training as will be continued and expanded through this renewal.

Public Health Relevance

TR&D2 will develop innovative NMR-compatible 3D cell and tissue culture and cell/tissue graft murine models of human disease and correlative pathology and biology methodologies and use them to develop and validate hyperpolarized molecular imaging probes that address important biomedical questions raised in the collaborative projects. Therefore this TR&D project aims to collaboratively develop new technology that through extensive dissemination and training will advance the field of hyperpolarized MR and improve patient care.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Biomedical Imaging and Bioengineering (NIBIB)
Type
Biotechnology Resource Grants (P41)
Project #
5P41EB013598-07
Application #
9324238
Study Section
Special Emphasis Panel (ZEB1-OSR-B)
Project Start
2011-08-01
Project End
Budget Start
2017-05-01
Budget End
2018-04-30
Support Year
7
Fiscal Year
2017
Total Cost
$316,265
Indirect Cost
$116,729

  Institution

Name
University of California San Francisco
Department
Type
Domestic Higher Education
DUNS #
094878337
City
San Francisco
State
CA
Country
United States
Zip Code
94118

  Publications

Milshteyn, Eugene; von Morze, Cornelius; Gordon, Jeremy W et al. (2018) High spatiotemporal resolution bSSFP imaging of hyperpolarized [1-13 C]pyruvate and [1-13 C]lactate with spectral suppression of alanine and pyruvate-hydrate. Magn Reson Med 80:1048-1060
von Morze, Cornelius; Reed, Galen D; Larson, Peder E et al. (2018) In vivo hyperpolarization transfer in a clinical MRI scanner. Magn Reson Med 80:480-487
Taglang, CĂ©line; Korenchan, David E; von Morze, Cornelius et al. (2018) Late-stage deuteration of 13C-enriched substrates for T1 prolongation in hyperpolarized 13C MRI. Chem Commun (Camb) 54:5233-5236
Gordon, Jeremy W; Hansen, Rie B; Shin, Peter J et al. (2018) 3D hyperpolarized C-13 EPI with calibrationless parallel imaging. J Magn Reson 289:92-99
Maidens, John; Gordon, Jeremy W; Chen, Hsin-Yu et al. (2018) Spatio-Temporally Constrained Reconstruction for Hyperpolarized Carbon-13 MRI Using Kinetic Models. IEEE Trans Med Imaging 37:2603-2612
Qin, Hecong; Carroll, Valerie N; Sriram, Renuka et al. (2018) Imaging glutathione depletion in the rat brain using ascorbate-derived hyperpolarized MR and PET probes. Sci Rep 8:7928
Marco-Rius, Irene; Gordon, Jeremy W; Mattis, Aras N et al. (2018) Diffusion-weighted imaging of hyperpolarized [13 C]urea in mouse liver. J Magn Reson Imaging 47:141-151
von Morze, Cornelius; Tropp, James; Chen, Albert P et al. (2018) Sensitivity enhancement for detection of hyperpolarized 13 C MRI probes with 1 H spin coupling introduced by enzymatic transformation in vivo. Magn Reson Med 80:36-41
Gordon, Jeremy W; Chen, Hsin-Yu; Autry, Adam et al. (2018) Translation of Carbon-13 EPI for hyperpolarized MR molecular imaging of prostate and brain cancer patients. Magn Reson Med :
Lee, Jessie E; Diederich, Chris J; Bok, Robert et al. (2018) Assessing high-intensity focused ultrasound treatment of prostate cancer with hyperpolarized 13 C dual-agent imaging of metabolism and perfusion. NMR Biomed :e3962

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