shot-button
E-paper E-paper
Home > Lifestyle News > Health And Fitness News > Article > Midlife blood test may predict cognitive decline Alzheimers later Study

Midlife blood test may predict cognitive decline, Alzheimer's later: Study

Updated on: 23 December,2023 11:13 AM IST  |  New York
IANS |

The new method opens a potentially powerful path to noninvasive, earlier detection and interventions for Alzheimer's disease and other dementias

Midlife blood test may predict cognitive decline, Alzheimer's later: Study

Image for representational purpose only. Photo Courtesy: istock

Researchers have connected two blood biomarkers to changes in cognitive function in women in midlife, opening a potentially powerful path to noninvasive, earlier detection and interventions for Alzheimer's disease and other dementias.


The study analysed two blood-based serum biomarkers, amyloid beta 42, 42/40 ratio, and phosphorylated tau181 (p-tau181), and tracked their levels in middle-aged women and compared results of a series of neurological function tests.


The analysis, published in the Alzheimer's & Dementia journal, found that higher levels of p-tau 181 were linked to accelerated cognitive decline and, likewise, lower amyloid beta 42/40 levels were associated with faster cognitive decline.


Their data came from 192 middle-aged women who were followed for 14 years.

"This is a new area of study, and it is very promising, but of course we are in need of a larger and more diverse sample," said Xin Wang, a research assistant professor in the Department of Epidemiology at the University of Michigan's School of Public Health. The findings suggest that midlife blood AD biomarker assessments may serve as early predictors of cognitive decline, offering an opportunity for early detection and prevention before development of irreversible dementia, Wang said.

Besides the possibility of earlier intervention for Alzheimer's disease and other forms of dementia, the blood biomarker tests such as those studied by the researchers could lead to less invasive, possibly more affordable methods of neurological testing, which currently calls for lumbar punctures for cerebral fluid and expensive PET scans for imaging.

"It's important to note that the presence of the biomarkers that we tested doesn't mean there is Alzheimer's Disease," Wang said.

"However, we know they are a central part of neuropathological changes. These pathological changes are important to know of earlier than later."

The researchers chose midlife as a "pivotal period" to test for and identify cognitive decline due to menopausal transition, which is characterised by sharp reduction in oestrogen levels and irreversible ovarian alterations and leads to changes in cognitive function.

In midlife, there is also a higher prevalence of cardiometabolic risk factors such as hypertension and diabetes, which are also associated with elevated risk of cognitive decline and dementia in older age.

Wang stressed that the findings are based on "only a very small sample, but the results are promising and an important building block for research with a larger, more diverse sample".

This story has been sourced from a third party syndicated feed, agencies. Mid-day accepts no responsibility or liability for its dependability, trustworthiness, reliability and data of the text. Mid-day management/mid-day.com reserves the sole right to alter, delete or remove (without notice) the content in its absolute discretion for any reason whatsoever.

"Exciting news! Mid-day is now on WhatsApp Channels Subscribe today by clicking the link and stay updated with the latest news!" Click here!

Register for FREE
to continue reading !

This is not a paywall.
However, your registration helps us understand your preferences better and enables us to provide insightful and credible journalism for all our readers.

Mid-Day Web Stories

Mid-Day Web Stories

This website uses cookie or similar technologies, to enhance your browsing experience and provide personalised recommendations. By continuing to use our website, you agree to our Privacy Policy and Cookie Policy. OK