Abstract
Abstract
There is evolving evidence that individuals categorized with subjective cognitive decline
(SCD) are potentially at higher risk for developing objective and progressive cognitive
impairment compared to cognitively healthy individuals without apparent subjective
complaints. Interestingly, SCD, during advancing preclinical Alzheimer’s disease (AD), may
denote very early, subtle cognitive decline that cannot be identified using established
standardized tests of cognitive performance. The substantial heterogeneity of existing
SCD-related research data has led the Subjective Cognitive Decline Initiative (SCD-I) to
accomplish an international consensus on the definition of a conceptual research framework
on SCD in preclinical AD. In the area of biological markers, the cerebrospinal fluid
signature of AD has been reported to be more prevalent in subjects with SCD compared to
healthy controls; moreover, there is a pronounced atrophy, as demonstrated by magnetic
resonance imaging, and an increased hypometabolism, as revealed by positron emission
tomography, in characteristic brain regions affected by AD. In addition, SCD individuals
carrying an apolipoprotein
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