TY - JOUR
T1 - Evolving Evidence for the Value of Neuroimaging Methods and Biological Markers in Subjects Categorized with Subjective Cognitive Decline.
AU - Lista, Simone
AU - Molinuevo, Jose L
AU - Cavedo, Enrica
AU - Rami, Lorena
AU - Amouyel, Philippe
AU - Teipel, Stefan J
AU - Garaci, Francesco
AU - Toschi, Nicola
AU - Habert, Marie-Odile
AU - Blennow, Kaj
AU - Zetterberg, Henrik
AU - O'Bryant, Sid E
AU - Johnson, Leigh
AU - Galluzzi, Samantha
AU - Bokde, Arun L W
AU - Broich, Karl
AU - Herholz, Karl
AU - Bakardjian, Hovagim
AU - Dubois, Bruno
AU - Jessen, Frank
AU - Carrillo, Maria C
AU - Aisen, Paul S
AU - Hampel, Harald
PY - 2015/9/24
Y1 - 2015/9/24
N2 - 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 ɛ4 allele are more likely to display AD-phenotypic alterations. The urgent requirement to detect and diagnose AD as early as possible has led to the critical examination of the diagnostic power of biological markers, neurophysiology, and neuroimaging methods for AD-related risk and clinical progression in individuals defined with SCD. Observational studies on the predictive value of SCD for developing AD may potentially be of practical value, and an evidence-based, validated, qualified, and fully operationalized concept may inform clinical diagnostic practice and guide earlier designs in future therapy trials.
AB - 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 ɛ4 allele are more likely to display AD-phenotypic alterations. The urgent requirement to detect and diagnose AD as early as possible has led to the critical examination of the diagnostic power of biological markers, neurophysiology, and neuroimaging methods for AD-related risk and clinical progression in individuals defined with SCD. Observational studies on the predictive value of SCD for developing AD may potentially be of practical value, and an evidence-based, validated, qualified, and fully operationalized concept may inform clinical diagnostic practice and guide earlier designs in future therapy trials.
KW - Alzheimer’s disease
KW - biological markers
KW - blood-based biomarkers
KW - cerebrospinal fluid biomarkers
KW - clinical trials
KW - functional MRI markers
KW - molecular imaging markers
KW - preclinical Alzheimer’s disease
KW - structural MRI markers
KW - subjective cognitive decline
U2 - 10.3233/JAD-150202
DO - 10.3233/JAD-150202
M3 - Article
C2 - 26402088
SN - 1875-8908
VL - 48 Suppl 1
JO - Journal of Alzheimer's disease : JAD
JF - Journal of Alzheimer's disease : JAD
ER -