- Toledo, Jon B;
- Zetterberg, Henrik;
- van Harten, Argonde C;
- Glodzik, Lidia;
- Martinez-Lage, Pablo;
- Bocchio-Chiavetto, Luisella;
- Rami, Lorena;
- Hansson, Oskar;
- Sperling, Reisa;
- Engelborghs, Sebastiaan;
- Osorio, Ricardo S;
- Vanderstichele, Hugo;
- Vandijck, Manu;
- Hampel, Harald;
- Teipl, Stefan;
- Moghekar, Abhay;
- Albert, Marilyn;
- Hu, William T;
- Argilés, Jose A Monge;
- Gorostidi, Ana;
- Teunissen, Charlotte E;
- De Deyn, Peter P;
- Hyman, Bradley T;
- Molinuevo, Jose L;
- Frisoni, Giovanni B;
- Linazasoro, Gurutz;
- de Leon, Mony J;
- van der Flier, Wiesje M;
- Scheltens, Philip;
- Blennow, Kaj;
- Shaw, Leslie M;
- Trojanowski, John Q
In a large multicentre sample of cognitively normal subjects, as a function of age, gender and APOE genotype, we studied the frequency of abnormal cerebrospinal fluid levels of Alzheimer's disease biomarkers including: total tau, phosphorylated tau and amyloid-β1-42. Fifteen cohorts from 12 different centres with either enzyme-linked immunosorbent assays or Luminex® measurements were selected for this study. Each centre sent nine new cerebrospinal fluid aliquots that were used to measure total tau, phosphorylated tau and amyloid-β1-42 in the Gothenburg laboratory. Seven centres showed a high correlation with the new Gothenburg measurements; therefore, 10 cohorts from these centres are included in the analyses here (1233 healthy control subjects, 40-84 years old). Amyloid-β amyloid status (negative or positive) and neurodegeneration status (negative or positive) was established based on the pathological cerebrospinal fluid Alzheimer's disease cut-off values for cerebrospinal fluid amyloid-β1-42 and total tau, respectively. While gender did not affect these biomarker values, APOE genotype modified the age-associated changes in cerebrospinal fluid biomarkers such that APOE ε4 carriers showed stronger age-related changes in cerebrospinal fluid phosphorylated tau, total tau and amyloid-β1-42 values and APOE ε2 carriers showed the opposite effect. At 40 years of age, 76% of the subjects were classified as amyloid negative, neurodegeneration negative and their frequency decreased to 32% at 85 years. The amyloid-positive neurodegeneration-negative group remained stable. The amyloid-negative neurodegeneration-positive group frequency increased slowly from 1% at 44 years to 16% at 85 years, but its frequency was not affected by APOE genotype. The amyloid-positive neurodegeneration-positive frequency increased from 1% at 53 years to 28% at 85 years. Abnormally low cerebrospinal fluid amyloid-β1-42 levels were already frequent in midlife and APOE genotype strongly affects the levels of cerebrospinal fluid amyloid-β1-42, phosphorylated tau and total tau across the lifespan without influencing the frequency of subjects with suspected non-amyloid pathology.