Holy, Emily Nicole; Li, Elizabeth; Bhattarai, Anjan; Fletcher, Evan; Alfaro, Evelyn R; Harvey, Danielle J; Spencer, Benjamin A; Cherry, Simon R; DeCarli, Charles S; Fan, Audrey P

doi:10.1186/s13550-024-01104-7

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Non-invasive quantification of 18F-florbetaben with total-body EXPLORER PET

2024

Published Web Location

https://doi.org/10.1186/s13550-024-01104-7

Abstract

Background

Kinetic modeling of ¹⁸F-florbetaben provides important quantification of brain amyloid deposition in research and clinical settings but its use is limited by the requirement of arterial blood data for quantitative PET. The total-body EXPLORER PET scanner supports the dynamic acquisition of a full human body simultaneously and permits noninvasive image-derived input functions (IDIFs) as an alternative to arterial blood sampling. This study quantified brain amyloid burden with kinetic modeling, leveraging dynamic ¹⁸F-florbetaben PET in aorta IDIFs and the brain in an elderly cohort.

Methods

¹⁸F-florbetaben dynamic PET imaging was performed on the EXPLORER system with tracer injection (300 MBq) in 3 individuals with Alzheimer's disease (AD), 3 with mild cognitive impairment, and 9 healthy controls. Image-derived input functions were extracted from the descending aorta with manual regions of interest based on the first 30 s after injection. Dynamic time-activity curves (TACs) for 110 min were fitted to the two-tissue compartment model (2TCM) using population-based metabolite corrected IDIFs to calculate total and specific distribution volumes (V_T, V_s) in key brain regions with early amyloid accumulation. Non-displaceable binding potential ([Formula: see text] was also calculated from the multi-reference tissue model (MRTM).

Results

Amyloid-positive (AD) patients showed the highest V_T and V_S in anterior cingulate, posterior cingulate, and precuneus, consistent with [Formula: see text] analysis. [Formula: see text]and V_T from kinetic models were correlated (r² = 0.46, P < 2[Formula: see text] with a stronger positive correlation observed in amyloid-positive participants, indicating reliable model fits with the IDIFs. V_T from 2TCM was highly correlated ([Formula: see text]= 0.65, P < 2[Formula: see text]) with Logan graphical V_T estimation.

Conclusion

Non-invasive quantification of amyloid binding from total-body ¹⁸F-florbetaben PET data is feasible using aorta IDIFs with high agreement between kinetic distribution volume parameters compared to [Formula: see text]in amyloid-positive and amyloid-negative older individuals.

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