4.6 Article

Performing radiosynthesis in microvolumes to maximize molar activity of tracers for positron emission tomography

Journal

COMMUNICATIONS CHEMISTRY
Volume 1, Issue -, Pages -

Publisher

NATURE PUBLISHING GROUP
DOI: 10.1038/s42004-018-0009-z

Keywords

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Funding

  1. National Institute of Biomedical Imaging and Bioengineering [R21 EB015540, T32 EB002101]
  2. National Institute on Aging [R21 AG049918]
  3. National Cancer Institute (Caltech/UCLA Nanosystems Biology Cancer Center) [U54 CA151819A]
  4. Department of Energy Office of Biological and Environmental Research [DE-SC0005056]
  5. UCLA Foundation
  6. NIH In Vivo Cellular and Molecular Imaging Centers Grant [P50 CA086306]
  7. NIH Cancer Center Support Grant [P30 CA016042]
  8. NIH SPORE Grant [P50 CA092131]

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Positron emission tomography (PET) is a molecular diagnostic imaging technology to quantitatively visualize biological processes in vivo. For many applications, including imaging of low-tissue density targets (e.g., neuroreceptors), imaging in small animals, and evaluation of novel tracers, the injected PET tracer must be produced with high molar activity to ensure low occupancy of biological targets and avoid pharmacologic effects. Additionally, high molar activity is essential for tracers with lengthy syntheses or tracers transported to distant imaging sites. Here we show that radiosynthesis of PET tracers in microliter volumes instead of conventional milliliter volumes results in substantially increased molar activity, and we identify the most relevant variables affecting this parameter. Furthermore, using the PET tracer [F-18]fallypride, we illustrate that molar activity can have a significant impact on biodistribution. With full automation, microdroplet platforms could provide a means for radiochemists to routinely, conveniently, and safely produce PET tracers with high molar activity.

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