Table 2.

PET biomarkers for neurodegenerative diseases

Biomarker	Target	Advantages	Disadvantages
18F-FDG	Glucose metabolism	Capable of detecting dysfunction that has not necessarily involved atrophy; well-validated for clinical research	Variability in methods of analysis between studies/centers
18F-FDDNP	AD lesions	18F half-life does not require on-site cyclotron	Does not differentiate Aβ or tau aggregations
11C-PBB3	Tau lesions	Sensitive to both AD-type tau aggregations and non-AD tau aggregations; correlates with clinical progression	Short half-life of 11C; relatively low affinity compared to other tau markers; non-specific binding
18F-AV1451 (flortaucipir)	Tau lesions	High affinity to aggregated tau; distribution of binding reflects clinical presentations; 18F half-life does not require on-site cyclotron	Off-target binding to neuromelanin and choroid plexus; poor reliability in early NFT stages; preferential binding to mixed 3R/4R tau rather than isolated 3R or 4R tau
18F-GTP1	Tau lesions	Ligand binding maps to known distribution of AD-tau aggregations; 18F half-life does not require on-site cyclotron	Yet to be fully validated; possible high non-specific binding in basal ganglia
18F-MK6240	Tau lesions	Extremely high binding affinity to tau aggregations; good brain delivery and washout; 18F half-life does not require on-site cyclotron	Likely preferential binding to mixed 3R/4R tau rather than isolated 3R or 4R tau; off-target binding to neuromelanin
18F-RO6958948	Tau lesions	High binding affinity to tau aggregations; preliminary study shows longitudinal increases in AD; 18F half-life does not require on-site cyclotron	Yet to be fully validated; no significant binding in 3R or 4R tauopathies
18F-THK5351	Tau lesions	High binding affinity to tau over Aβ aggregations; 18F half-life does not require on-site cyclotron	High non-specific retention in the subcortical white matter; high MOA-B binding
18F-THK5105	Tau lesions	High binding affinity to tau over Aβ aggregations; 18F half-life does not require on-site cyclotron	High non-specific retention in the subcortical white matter; inferior signal-to-background ratio
18F-THK523	Tau lesions	High binding affinity to tau over Aβ aggregations; 18F half-life does not require on-site cyclotron	High non-specific retention in the subcortical white matter; poor in vivo visualization of tau deposition
18F-PI2620	Tau lesions	Binds to both 3R/4R mix tau and 3R tau (Pick’s disease); high binding affinity to tau over Aβ aggregations and MOA-A/MOA-B; 18F half-life does not require on-site cyclotron	Yet to be fully validated
18F-PM-PBB3	Tau lesions	Indication that ligand is sensitive to both AD and non-AD tauopathies; little binding to MOA-A and MOA-B; 18F half-life does not require on-site cyclotron	Yet to be fully validated, particularly in non-AD tauopathies
11C-PiB	Amyloid-β aggregations	High affinity to fibrillar Aβ; best studied of available Aβ PET tracers	Short half-life of 11C; not specific to AD amyloidosis/binds to CAA
18F-AV-45	Amyloid-β aggregations	High affinity to fibrillar Aβ; 18F half-life does not require on-site cyclotron	Not specific to AD amyloidosis
18F-BAY94-9172 (florbetaben)	Amyloid-β aggregations	High affinity to fibrillar Aβ; 18F half-life does not require on-site cyclotron	Not specific to AD amyloidosis
18F-GE067 (flutemetamol)	Amyloid-β aggregations	High affinity to fibrillar Aβ; 18F half-life does not require on-site cyclotron	Not specific to AD amyloidosis
18F-NAV4694	Amyloid-β aggregations	Excellent agreement with 11C-PiB; 18F half-life does not require on-site cyclotron	Not specific to AD amyloidosis
11C-UCB-J	Synapses (SV2A)	High affinity to protein expressed on synapses	Short half-life of 11C; relatively new tracer and not well-validated in dementia populations

Abbreviations: PET positron emission tomography, FTD frontotemporal dementia, MOA-B monoamine oxidase B, PiB Pittsburg Compound-B, CAA cerebral amyloid angiopathy, FDG fluorodeoxyglucose, SV2A synaptic vesicle glycoprotein 2A