Cerebrospinal fluid and plasma biomarkers in individuals at risk for genetic prion disease.
Sonia M VallabhEric Vallabh MinikelVictoria J WilliamsBecky C CarlyleAlison J McManusChase D WennickAnna BollingBianca A TrombettaDavid UrickChloe K NobuharaJessica GerberHolly DuddyIngolf LachmannChristiane StehmannSteven J CollinsKaj BlennowHenrik ZetterbergSteven E ArnoldPublished in: BMC medicine (2020)
CSF PrP will be interpretable as a pharmacodynamic readout for PrP-lowering therapeutics in pre-symptomatic individuals and may serve as an informative surrogate biomarker in this population. In contrast, markers of prion seeding activity and neuronal damage do not reliably cross-sectionally distinguish mutation carriers from controls. Thus, as PrP-lowering therapeutics for prion disease advance, "secondary prevention" based on prodromal pathology may prove challenging; instead, "primary prevention" trials appear to offer a tractable paradigm for trials in pre-symptomatic individuals.