[(18)F]tetrafluoroborate as a PET tracer for the sodium/iodide symporter: the importance of specific activity

Alex Khoshnevisan; Maite Jauregui-Osoro; Karen Shaw; Julia Baguña Torres; Jennifer D Young; Nisha K Ramakrishnan; Alex Jackson; Gareth E Smith; Antony D Gee; Philip J Blower

doi:10.1186/s13550-016-0188-5

[(18)F]tetrafluoroborate as a PET tracer for the sodium/iodide symporter: the importance of specific activity

EJNMMI Res. 2016 Dec;6(1):34. doi: 10.1186/s13550-016-0188-5. Epub 2016 Apr 22.

Affiliations

¹ Division of Imaging Sciences and Biomedical Engineering, King's College London, 4th Floor Lambeth Wing, St. Thomas' Hospital, London, SE1 7EH, UK.
² The Grove Centre, GE Healthcare, White Lion Road, Amersham, UK.
³ Division of Imaging Sciences and Biomedical Engineering, King's College London, 4th Floor Lambeth Wing, St. Thomas' Hospital, London, SE1 7EH, UK. [email protected].

Abstract

Background: [(18)F]BF4 (-), the first (18)F-labelled PET imaging agent for the sodium/iodide symporter (NIS), was produced by isotopic exchange yielding a product with limited specific activity (SA, ca. 1 GBq/μmol) posing a risk of sub-optimal target-to-background ratios (TBR) in PET images due to saturation of NIS in vivo. We sought to quantify this risk and to develop a method of production of [(18)F]BF4 (-) with higher SA.

Methods: A new radiosynthesis of [(18)F]BF4 (-) was developed, involving reaction of [(18)F]F(-) with boron trifluoride diethyl etherate under anhydrous conditions, guided by (11)B and (19)F NMR studies of equilibria involving BF4 (-) and BF3. The SA of the product was determined by ion chromatography. The IC50 of [(19)F]BF4 (-) as an inhibitor of [(18)F]BF4 (-) uptake was determined in vitro using HCT116-C19 human colon cancer cells expressing the human form of NIS (hNIS). The influence of [(19)F]BF4 (-) dose on biodistribution in vivo was evaluated in normal mice by nanoPET imaging and ex vivo tissue counting.

Results: An IC50 of 4.8 μΜ was found in vitro indicating a significant risk of in vivo NIS saturation at SA achieved by the isotopic exchange labelling method. In vivo thyroid and salivary gland uptake decreased significantly with [(19)F]BF4 (-) doses above ca. 10 μg/kg. The new radiosynthesis gave high radiochemical purity (>99 %) and moderate yield (15 %) and improved SA (>5 GBq/μmol) from a starting activity of only 1.5 GBq.

Conclusions: [(18)F]BF4 (-) produced at previously reported levels of SA (1 GBq/μmol) can lead to reduced uptake in NIS-expressing tissues in mice. This is much less likely in humans. The synthetic approach described provides an alternative for production of [(18)F]BF4 (-) at higher SA with sufficient yield and without need for unusually high starting activity of [(18)F]fluoride, removing the risk of NIS saturation in vivo even in mice.

Trial registration: ISRCTN75827286 .

Keywords: Fluorine-18; PET; Sodium/iodide symporter; Specific activity; Tetrafluoroborate; Thyroid.

[(18)F]tetrafluoroborate as a PET tracer for the sodium/iodide symporter: the importance of specific activity

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Abstract

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