Evaluation of [18F] FNM biodistribution and dosimetry based on whole-body PET imaging of rats
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Salabert, Anne Sophie
Mora Ramírez, Erick
Beaurain, Marie
Alonso, Mathieu
Fontan, Charlotte
Tahar, Hafid Belhadj
Boizeau, Marie Laure
Tafani, Mathieu
Bardiès, Manuel
Payoux, Pierre
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Abstract
Introduction: The aim of this work was to study the biodistribution, metabolism and radiation dosimetry of rats
injected with [18F]FNM using PET/CT images. This novel radiotracer targeting NMDA receptor has potential for
investigation for neurological and psychiatric diseases.
Methods: Free fraction and stability in fresh human plasma were determined in vitro. PET/CT was performed on
anesthetized rats. Organs were identified and 3D volumes of interest (VOIs) were manually drawn on the CT in
the center of each organ. Time activity curves (TACs) were created with these VOIs, enabling the calculation of
residence times. To confirm these values, ex vivo measurements of organs were performed. Plasma and urine
were also collected to study in vivo metabolism. Data was extrapolated to humans, effective doses were estimat ed using ICRP-60 and ICRP-89 dosimetric models and absorbed doses were estimated using OLINDA/EXM V1.0
and OLINDA/EXM V2.0 (which use weighting factors from ICRP-103 to do the calculations).
Results: The [18F]FNM was stable in human plasma and the diffusible free fraction was 53%. As with memantine,
this tracer is poorly metabolized in vivo. Ex vivo distributions validated PET/CT data as well as demonstrating a
decrease of radiotracer uptake in the brain due to anesthesia. Total effective dose was around 6.11 μSv/MBq
and 4.65 μSv/MBq for female and male human dosimetric models, respectively.
Conclusions: This study shows that the presented compound exhibits stability in plasma and plasma protein bind ing very similar to memantine. Its dosimetry shows that it is suitable for use in humans due to a low total effective
dose compared to other PET radiotracers.
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Keywords
Dosimetry, [18F] FNM, Position emission tomography (PET), NMDA receptor, OLINDA, RADIACIÓN, CANCER
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https://www.sciencedirect.com/science/article/pii/S0969805117303633?via%3Dihub
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