| Literature DB >> 21047401 |
Felix Bermejo-Pareja1, Desiree Antequera, Teo Vargas, Jose A Molina, Eva Carro.
Abstract
BACKGROUND: Simple, non-invasive tests for early detection of degenerative dementia by use of biomarkers are urgently required. However, up to the present, no validated extracerebral diagnostic markers for the early diagnosis of Alzheimer disease (AD) are available. The clinical diagnosis of probable AD is made with around 90% accuracy using modern clinical, neuropsychological and imaging methods. A biochemical marker that would support the clinical diagnosis and distinguish AD from other causes of dementia would therefore be of great value as a screening test. A total of 126 samples were obtained from subjects with AD, and age-sex-matched controls. Additionally, 51 Parkinson's disease (PD) patients were used as an example of another neurodegenerative disorder. We analyzed saliva and plasma levels of β amyloid (Aβ) using a highly sensitive ELISA kit.Entities:
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Year: 2010 PMID: 21047401 PMCID: PMC2987856 DOI: 10.1186/1471-2377-10-108
Source DB: PubMed Journal: BMC Neurol ISSN: 1471-2377 Impact factor: 2.474
Demographic and health characteristics of the final sample (n = 136)
| Mean age | Sex | Mean MMSE | Mean onset | |
|---|---|---|---|---|
| AD patients | 77.20 (60-91) | 21/49 | 17 (4-28) | 2.56 (0-12) |
| PD patients | 72.96 (60-93) | 26/25 | 28 (22-30) | 3.8 (1-5) |
| Control subjects | 74.35 (64-85) | 17/39 | nd |
MMSE = mini-mental state examination; AD = Alzheimer's disease; PD = Parkinson's disease; nd = not determined.
Saliva Aβ42 levels in patients with neurodegenerative diseases and control subjects
| Group | Aβ42 (pg/ml) | Aβ40 (pg/ml) | No. of subjects |
|---|---|---|---|
| AD patients | 70 | ||
| Mild | 7.67 ± 16.25* | 21.87 ± 5.7 | 29 |
| Moderate | 11.70 ± 34.76 | 21.5 ± 4.17 | 24 |
| Severe | 3.03 ± 3.49 | 23.92 ± 4.55 | 17 |
| PD patients | 3.66 ± 4.21 | 26.41 ± 5.12 | 51 |
| Control subjects | 2.89 ± 4.96 | 20.82 ± 5.55 | 56 |
AD = Alzheimer's disease; PD = Parkinson's disease. Values are mean ± SD. *p < 0.05 versus control subjects
Saliva Aβ42 levels in patients with AD and control subjects
| Group | No. Of subjects | Age | Aβ42 (pg/ml) |
|---|---|---|---|
| AD patients | 38 | ||
| With Apo E ε4 | 18 | 75.18 ± 7.91 | 6.42 ± 15.48 |
| Without Apo E ε4 | 20 | 75.05 ± 8.85 | 12.52 ± 33.58 |
| Control subjects | 34 | ||
| With Apo E ε4 | 4 | 68.5 ± 8.70 | 2.05 ± 1.48 |
| Without Apo E ε4 | 30 | 69.10 ± 9.25 | 2.51 ± 2.61 |
Data are mean ± SD; AD = Alzheimer's disease.
Figure 1Western-blot analysis of saliva levels of gelsolin (. Figures shows representative blots and quantitative from 4 independent measurements.