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Logo of alzrethBioMed CentralBiomed Central Web Sitesearchsubmit a manuscriptregisterthis articleAlzheimer's Research & TherapyJournal Front Page
 
Alzheimers Res Ther. 2011; 3(6): 33.
Published online 2011 November 25. doi:  10.1186/alzrt95
PMCID: PMC3308022
Copyright ©2010 BioMed Central Ltd
Predicting Alzheimer's risk: why and how?
Deborah E Barnescorresponding author1,2,3 and Sei J Lee2,4
1Department of Psychiatry, University of California at San Francisco, San Francisco, CA, USA
2Health Services Research, Mental Health Service, San Francisco VA Medical Center, 4150 Clement Street (151R), San Francisco, CA 94121, USA
3Program for the Aging Century, Division of Geriatrics, Department of Medicine, University of California at San Francisco, San Francisco, CA 94118, USA
4Division of Geriatrics, Department of Medicine, University of California at San Francisco, San Francisco, CA 94118, USA
corresponding authorCorresponding author.
Deborah E Barnes: deborah.barnes/at/ucsf.edu; Sei J Lee: sei.lee/at/ucsf.edu
Abstract
Because the pathologic processes that underlie Alzheimer's disease (AD) appear to start 10 to 20 years before symptoms develop, there is currently intense interest in developing techniques to accurately predict which individuals are most likely to become symptomatic. Several AD risk prediction strategies - including identification of biomarkers and neuroimaging techniques and development of risk indices that combine traditional and non-traditional risk factors - are being explored. Most AD risk prediction strategies developed to date have had moderate prognostic accuracy but are limited by two key issues. First, they do not explicitly model mortality along with AD risk and, therefore, do not differentiate individuals who are likely to develop symptomatic AD prior to death from those who are likely to die of other causes. This is critically important so that any preventive treatments can be targeted to maximize the potential benefit and minimize the potential harm. Second, AD risk prediction strategies developed to date have not explored the full range of predictive variables (biomarkers, imaging, and traditional and non-traditional risk factors) over the full preclinical period (10 to 20 years). Sophisticated modeling techniques such as hidden Markov models may enable the development of a more comprehensive AD risk prediction algorithm by combining data from multiple cohorts. As the field moves forward, it will be critically important to develop techniques that simultaneously model the risk of mortality as well as the risk of AD over the full preclinical spectrum and to consider the potential harm as well as the benefit of identifying and treating high-risk older patients.
 
There is a growing recognition that the complex pathologic cascade that leads to Alzheimer's disease (AD) begins decades before the development of clinical symptoms [1]. This suggests that effective prevention will require predicting who will develop AD decades before the onset of symptoms. Therefore, there has been growing interest in developing accurate ways of identifying individuals who have an increased risk of developing symptomatic AD so that they can be targeted for preventive interventions such as risk factor reduction, behavioral modification, or pharmacologic treatment.
Much of the current work on AD prediction, including the Alzheimer's Disease Neuroimaging Initiative (ADNI), has focused on identifying biomarkers and neuroimaging tests that can accurately detect individuals with preclinical disease. These approaches implicitly recognize the multifaceted nature of the AD pathologic cascade (amyloid beta deposition, neurofibrillary tangles, neuronal dysfunction, and cerebral volume loss) [2] and rely on different tests to capture different aspects of that pathology. One recent analysis of ADNI data [3] found that a combination of magnetic resonance imaging (MRI), cerebrospinal fluid, and neuropsychological and functional markers predicted conversion from mild cognitive impairment to AD with moderate accuracy (c statistic = 0.80). The c statistic, also known as the area under the receiver operating characteristic curve, may range from 0 to 1, with 1 reflecting perfect discrimination and 0.5 reflecting no better than chance.
An alternative approach to the prediction of AD risk has been to identify combinations of traditional risk factors that can reliably differentiate individuals with a high risk of developing AD from those with a low risk. One study found that mid-life risk factors, including age, education, hypertension, hypercholesterolemia, and obesity, predicted late-life dementia risk with moderate accuracy (c statistic = 0.77) [4]. Another study found that a combination of late-life factors, including age, cognitive test scores, MRI measures, apolipoprotein E (APOE) genotype, cardiovascular disease, and functional measures, also predicted dementia risk with moderate accuracy (c statistic = 0.82) [5]. An abbreviated version that included age and simplified measures of cognitive function and cardiovascular disease had moderate accuracy as well (c statistic = 0.77) [6].
Another recent study extended this work by noting that a tremendous range of factors appear to predict AD, suggesting that AD is more likely in people with a broad decline in health. Song and colleagues [7] found that 19 non-traditional risk factors such as a general health question ('How good is your health?') and sensory questions ('How good is your eyesight or hearing?') predicted which individuals were likely to develop AD, even after accounting for traditional risk factors such as age, sex, education, cognitive function, and cardiovascular disease. Implicit in this study is the assumption that, before leading to symptoms of cognitive impairment, AD is associated with non-specific symptoms such as worse self-rated health. However, the prognostic accuracy of this model was only fair (c statistic = 0.66). In fact, in another study, demographics alone were found to be more predictive of dementia risk (c statistic = 0.72), and significant increases in prognostic accuracy were associated with the addition of APOE genotype (c statistic = 0.75) and vascular risk factors (c statistic = 0.79) [8].
Taken together, these studies suggest that there are a variety of approaches for identifying with fair to moderate levels of discrimination those individuals who are at high risk of developing AD. However, all of these models suffer from two important limitations in their approach to the prediction of AD risk.
First, none of these models explicitly accounts for the competing risk of death. AD is predominantly a disease of older adults who experience high rates of death from other causes. To effectively target preventive interventions - in particular, pharmacologic interventions that may have adverse side effects - AD prediction models must identify individuals who are likely to suffer symptomatic AD before death. Many risk factors for AD are also risk factors for mortality (for example, older age, vascular risk factors, and functional limitations) [9]. Therefore, some patients who are at high risk for AD may be at even higher risk for death before symptomatic AD. To appropriately balance the potential benefit of preventive intervention with the potential harm, AD prediction models must account for death and identify individuals whose risk of AD outweighs their risk of death.
Second, dementia risk models developed to date have been developed in cohort studies that focused on a limited range of potential predictors and had relatively short follow-up periods (<10 years) or relatively narrow risk windows (for example, mid-life only and late-life only). Thus, these studies have not examined the full range of AD predictors (biomarkers, neuroimaging techniques, and traditional and non-traditional risk factors) over the full 10-to 20-year preclinical risk period. The ideal study would include repeated ascertainment of thousands of individuals over several decades, requiring a tremendous investment in resources. Furthermore, these prospectively collected data would not be available for decades, suggesting that alternative modeling techniques need to be employed. One possible solution is to use hidden Markov models [10], which potentially could be used to combine data from multiple sources to model disease state transitions across the full AD clinical-pathologic spectrum.
In conclusion, prediction of AD risk is a relatively new field of inquiry. Several alternative approaches with moderate levels of accuracy have been developed, but none is ready for widespread clinical use. As the field moves forward, it will be critically important to develop techniques that simultaneously model the risk of mortality as well as the risk of AD over the full preclinical spectrum and to consider the potential harm as well as the benefit of identifying and treating high-risk older patients.
Abbreviations
AD: Alzheimer's disease; ADNI: Alzheimer's Disease Neuroimaging Initiative; APOE: apolipoprotein E; MRI: magnetic resonance imaging.
Competing interests
The authors declare that they have no competing interests.
Acknowledgements
This work was supported in part by funding from the S. D. Bechtel, Jr. Foundation, including an Early Investigator award (principal investigator: SJL), and the Program for the Aging Century. SJL was also supported by a Paul Beeson Career Development Award from the National Institute on Aging and the American Federation for Aging Research (K23AG040779). Funders were not involved in the conception of this work, writing of the manuscript, or the decision to submit the manuscript for publication.
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