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Demographic data, imaging results, biomarkers of study participants help determine risk
When people participate in studies of aging, they often want to know what their individual risks of developing dementia from Alzheimers disease are. Washington University researchers have developed an algorithm that can help provide them with information about what their risks may be.
Using demographic information, brain imaging test results and genetic biomarkers, researchers at Washington University School of Medicine in St. Louis have developed an algorithm that can help provide people who volunteer for studies of aging with information about the risk each faces of developing dementia due to Alzheimers disease.
Published Sept. 30 in the Journal of Alzheimers and Dementia, the findings from researchers with the universitys Knight Alzheimer Disease Research Center (Knight ADRC) may help study participants learn more about what their futures hold, in terms of risk for dementia related to Alzheimers. The research also eventually may help others determine whether they face risk of the debilitating disorder.
Thousands of adults have volunteered for studies at Alzheimers research centers around the country, said principal investigator Sarah M. Hartz, MD, PhD, an associate professor of psychiatry. They come back and undergo tests year after year, including PET (positron emission tomography) and MRI scans, blood draws, cognitive tests, and lumbar punctures that measure proteins in spinal fluid. Those studies advance the overall understanding of Alzheimers disease, but they give participants relatively little information about their own risk. This algorithm is a way to help illuminate that information and to let individuals know whether they have a significant risk for dementia related to Alzheimers disease.
Hartz and co-principal investigator Jessica Mozersky, PhD, an assistant professor of medicine in the universitys Bioethics Research Center, examined the various factors that contribute to Alzheimers dementia, and they used that information to create an algorithm aimed at estimating an individuals absolute risk of developing early symptoms of dementia from Alzheimers. They developed the algorithm for use in a clinical trial to learn whether they could help volunteers participating in aging studies at the Knight ADRC better understand what biomarkers for disease they might have, and whether researchers then could evaluate participants eventual outcomes.
We developed the algorithm because study participants wanted more than just a report of whether their test results were normal or abnormal, Mozersky said. Weve performed studies with people who receive results reporting elevated amyloid, for example. They tell us, You know what I really want to know? My risk.
The website with the risk algorithm uses demographic information, along with specific test results, to help study volunteers better understand their risk.
Over the years, there have been ethical debates about how much information to release to people who participate in such studies because there arent yet any treatments to prevent or cure Alzheimers dementia. Further, how well various biomarkers predict the problem in people who have no symptoms of the disorder has not been well studied.
We developed the algorithm so that we can tell participants what currently is known in a meaningful way, and so that the algorithm can be updated easily as new research or data emerges, Hartz said.
The algorithm, accessible on the Knight ADRCs website at https://alzheimerdementiacalculator.wustl.edu/, provides greater detail for researchers and individuals who want to learn more about Alzheimers dementia risk. For example, a 69-year-old woman who went to college and had a parent with dementia from Alzheimers has about a 6% risk of developing the early symptoms of Alzheimers dementia in the next five years. That, of course, means she also has a 94% chance of not developing dementia from Alzheimers in the next five years.
The algorithm incorporates amyloid PET scan results and brain hippocampal volumes a smaller hippocampus often suggests an increased risk for damage related to Alzheimers dementia to show how risk changes when such extra information is known. If that same 69-year-old woman also had a PET scan revealing elevated levels of amyloid, and a decrease in hippocampal volume, her risk would rise to about 33%.
Still, age is the biggest demographic risk factor, Hartz said.
If the woman was 85 years old rather than 69, her risk of developing dementia from Alzheimers in the next five years would climb from about 6% to about 32%, even without knowing any biomarker-related results.
The researchers also looked at a gene known to influence risk of Alzheimers dementia. Risk increases significantly depending on the type of APOE gene a person has. But when the researchers included APOE genotype in their model, they found it didnt tell them anything that data from imaging tests hadnt already revealed. This is likely because brain changes seen on imaging tests occur in part because of the APOE gene.
Hartz and Mozersky are continuing their work to improve the ability to predict Alzheimers dementia risk based on these variables. They have grants totaling more than $5 million from the National Institute on Aging to run a clinical trial to better understand the impact of providing these risk assessments to people participating in research and to validate their algorithm in larger samples.
Researchers worry about how such information will affect study participants, Hartz said. We want to learn how the information might affect them and whether providing this sort of information actually may help them.
Hartz SM, Mozersky J, Schindler SE, Linnenbringer E, Wang J, Gordon BA, Raji CA, Moulder KL, West T, Benzinger TLS, Cruchaga C, Hassenstab JJ, Bierut LJ, Xiong C, Morris JC. A flexible modeling approach for biomarker-based computation of absolute risk of Alzheimer disease dementia. The Journal of Alzheimers and Dementia, Sept. 30, 2022.
This work is supported by the National Institute on Aging and the National Cancer Institute of the National Institutes of Health (NIH). Grant numbers include R01 AG065234, P01 AG026276, 5P01 AG003991, P30 AG066444, 1UL1 TR002345, R44 AG059489, R01 AG07094 and U01 AG016976, with additional grants that provide funding for the Alzheimers Disease Research Centers involved in these studies (for a complete list, refer to the paper). Other funding sources include BrightFocus CA2016636, the Gerald and Henrietta Rauenhorst Foundation and the Alzheimers Drug Discovery Foundation.
About Washington University School of Medicine
WashU Medicine is a global leader in academic medicine, including biomedical research, patient care and educational programs with 2,700 faculty. Its National Institutes of Health (NIH) research funding portfolio is the fourth largest among U.S. medical schools, has grown 54% in the last five years, and, together with institutional investment, WashU Medicine commits well over $1 billion annually to basic and clinical research innovation and training. Its faculty practice is consistently within the top five in the country, with more than 1,790 faculty physicians practicing at over 60 locations and who are also the medical staffs of Barnes-Jewish and St. Louis Childrens hospitals of BJC HealthCare. WashU Medicine has a storied history in MD/PhD training, recently dedicated $100 million to scholarships and curriculum renewal for its medical students, and is home to top-notch training programs in every medical subspecialty as well as physical therapy, occupational therapy, and audiology and communications sciences.
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