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

Author:

Holy Emily Nicole1ORCID,Li Elizabeth2,Bhattarai Anjan3,Fletcher Evan4,Alfaro Evelyn R.4,Harvey Danielle J.5,Spencer Benjamin A.6,Cherry Simon R.6,DeCarli Charles S.4,Fan Audrey P.3

Affiliation:

1. UC Davis: University of California Davis

2. University of Pennsylvania Department of Medicine

3. University of California Davis Department of Biomedical Engineering

4. University of California Davis Department of Neurology

5. University of California Davis Department of Public Health Sciences

6. University of California Davis Department of Radiology

Abstract

Abstract Purpose 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 seconds after injection. Dynamic time-activity curves (TACs) for 110 minutes were fitted to the two-tissue compartment model (2TCM) using population-based metabolite corrected IDIFs to calculate total and specific distribution volumes (VT, Vs) in key brain regions with early amyloid accumulation. Non-displaceable binding potential (\({BP}_{ND})\) was also calculated from the multi-reference tissue model (MRTM). Results Amyloid-positive (AD) patients showed the highest VT and VS in anterior cingulate, posterior cingulate, and precuneus, consistent with \({BP}_{ND}\) analysis. \({BP}_{ND}\)and VT from kinetic models were correlated (r² = 0.46, P < 2\({e}^{-16})\) with a stronger positive correlation observed in amyloid-positive participants, indicating reliable model fits with the IDIFs. VT from 2TCM was highly correlated (\({r}^{2}\)= 0.65, P < 2\({e}^{-16}\)) with Logan graphical VT 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 \({BP}_{ND}\)in amyloid-positive and negative older individuals.

Publisher

Research Square Platform LLC

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