Table 1.
Comparison of different aspects relevant for implementation of Aβ-PET, CSF, and blood-based analysis methods
| Topic | Aβ-PET imaging | CSF analysis | Blood analysis |
|---|---|---|---|
| Context of use (COU) | Used in clinical trials as an entry point for patient stratification with the aim to identify subjects with Aβ load in the brain [73] | More applications: early diagnosis, differential diagnosis, treatment follow-up |
Multiple applications in the diagnostic or therapeutic area, including (pre-) clinical studies (PK/PD testing) Biomarkers can be disease-related or treatment-related, classified by the BEST biomarker category (Web-1) |
|
Clinical Method comparison |
Both methods have a high clinical accuracy to identify Aβ load in the brain. Concordance between results is high, although discrepant results have been published | Correlation with CSF for some proteins (e.g., NF-L, Aβ ratio), not for other proteins | |
| Comparison needs to be done with respect to the clinical utility or for a specific COU | |||
| Possibility for use of blood protein panels in combination with other diagnostic tools (e.g., CSF) [21] | |||
|
Clinical Change in function of disease process |
Aβ-PET scan differences are visualized after changes in CSF biomarker profiles | Changes in concentrations of CSF proteins are detectable more than 20 years before cognitive symptoms appear | To be defined, as compared to Aβ-PET imaging or CSF analysis |
| Comparison is dependent on the COU | |||
| Clinical trials | Used for patient stratification | Exploratory biomarker | Not integrated in trials yet |
| Analytes_number |
One hallmark. Different outcome in function of the selected tracer |
Several relevant proteins can be included in the panel (e.g., tau, Aβ, NF-L, …) | A huge number of proteins can be included in the panel |
| Most proteins are detectable with classical technology platforms | Concentrations are lower than in CSF (for most of the analytes), but technologies allow low limit of detection | ||
| Cost | High cost, limiting repeated measures | Limited cost/sample | Low cost/sample |
| Repeated sampling is possible, but more difficult | Repeated sampling is possible | ||
| Safety | Exposure to radiation. Problems with claustrophobia for demented subject | Lumbar Puncture is perceived as invasive and with a risk of 1–5% for severe headache problems [59] | Safe, routine procedure |
| Instrumentation |
PET scanners: not available worldwide Cyclotrons: tracers need to be on-site within 1 h of preparation |
Random-access immunoassay analyzers have been qualified for accurate and reliable quantification of CSF proteins [9] | Point-of-care test systems for multiple protein analysis will become available soon. Random-access analyzers are already available in many labs |
| Technology is only available in specialized centers | |||
|
Standardization Training |
It needs to be performed independent of a patient’s clinical feature. Only by readers who successfully complete a special training program |
CSF-Aβ1–42 data can be harmonized between technology platforms using CSF-based certified reference materials [32] Efforts are ongoing for a worldwide implementation of a SOP for collection and storage of CSF. Run-validation criteria can be established easily. Each lab technician, skilled in the art, can perform these immunoassays |
No special training required, except availability of technicians, skilled in the art to perform immunoassays |
| Data interpretation | Visual interpretation or software. Flashy outcome | Reader and curve fit algorithms. Objective outcome. Interpretation is more difficult. No universal cutoff value available | |
| Regulatory | The FDA approved Aβ-PET imaging by visual interpretation (‘not software’) to identify subjects with ongoing amyloidopathy (= exclusion criterium) [73] |
EMA qualified the combined use of CSF Aβ and tau proteins as a tool for patient enrollment in clinical trials (Web-2) A letter of support from the FDA encourages their use in clinical trials (Web-3). The method must be used in adjunct to other diagnostic evaluations. Algorithms based on CSF proteins, together with imaging methods, were integrated into revised criteria for AD diagnosis [18] and research proposals for the amyloid/tau/neurodegeneration (A/T/N) classification of AD pathological processes [27] |
No qualification proposals submitted |
| No regulatory approved assay formats | |||
Website references: Web-1 https://www.ncbi.nlm.nih.gov/books/NBK326791/; Web-2 https://www.ema.europa.eu/en/documents/regulatory-procedural-guideline/qualification-opinion-novel-methodologies-predementia-stage-alzheimers-disease-cerebrospinal-fluid_en.pdf; Web-3 https://www.fda.gov/drugs/cder-biomarker-qualification-program/letter-support-los-initiative
Aβ β-amyloid, COU context of use, CSF cerebrospinal fluid, EMA the European Medicine Agency, FDA The Food and Drug Administration, NF-L neurofilament light, PET positron emission tomography, SOP standard operating procedure