Summary: A new study finds that higher inflammation in young adulthood is associated with reduced cognitive function in midlife. Researchers discovered that inflammation due to factors like obesity and smoking can impact memory and processing speed.
This link, previously noted in older adults, now extends to early adulthood, suggesting long-term brain health effects. Reducing inflammation through lifestyle changes may help prevent cognitive decline.
Key Facts:
- Inflammation’s Impact: Higher inflammation in young adults linked to lower cognitive performance in midlife.
- Study Data: Followed 2,364 adults over 18 years, measuring inflammation and cognitive skills.
- Preventive Measures: Physical activity and quitting smoking can reduce inflammation and potentially prevent cognitive decline.
Source: UCSF
Higher inflammation in young adulthood linked to lower performance in skills testing in midlife.
Young adults who have higher levels of inflammation, which is associated with obesity, physical inactivity, chronic illness, stress and smoking, may experience reduced cognitive function in midlife, a new study out of UC San Francisco has found.
Researchers previously linked higher inflammation in older adults to dementia, but this is one of the first studies to connect inflammation in early adulthood with lower cognitive abilities in midlife.
“We know from long-term studies that brain changes leading to Alzheimer’s disease and other dementias may take decades to develop,” said first author Amber Bahorik, PhD, of the UCSF Department of Psychiatry and Behavioral Sciences and the Weill Institute for Neurosciences.
“We wanted to see if health and lifestyle habits in early adulthood may play a part in cognitive skills in midlife, which in turn may influence the likelihood of dementia in later life.”
In their study, publishing in Neurology on July 3, researchers found that only 10% of those with low inflammation performed poorly on testing of processing speed and memory, compared to 21% and 19%, respectively, of those with either moderate or higher levels of inflammation.
When researchers adjusted for factors like age, physical activity and total cholesterol, disparities remained in processing speed; and the researchers also found differences in executive functioning, which includes working memory, problem solving and impulse control.
The study followed 2,364 adults in the CARDIA study, which aims to identify the factors in young adulthood that lead to cardiovascular disease two-to-three decades later.
Participants were 18 to 30 years old when they entered the study and were tested four times over an 18-year period for the inflammatory marker C-reactive protein (CRP). They took the cognitive tests five years after their last CRP measurement, by which time most participants were in their forties and fifties.
About half the participants were female; a little under half were Black, and the rest were white. Some 45% had lower stable inflammation, while 16% had moderate or increasing inflammation; 39% had higher levels.
A link between inflammation and health risks
The researchers also linked higher levels of inflammation with physical inactivity, higher BMI and current smoking.
“Inflammation plays a significant role in cognitive aging and may begin in early adulthood,” said senior author Kristine Yaffe, MD, a professor of psychiatry and behavioral sciences, neurology, and epidemiology and biostatistics at UCSF. “There is likely a direct and indirect effect of inflammation on cognition.”
Yaffe is a member of the first team of experts to determine that 30% of dementia risk is preventable. Her recent research has looked at the association in midlife between fragmented sleep and lower cognition and the effects of personalized health and lifestyle changes in preventing memory loss in higher-risk older adults.
“Fortunately, there are ways to reduce inflammation – such as by increasing physical activity and quitting smoking – that might be promising paths for prevention,” Yaffe said.
Co-Authors: Tina Hoang, MSPH, of Northern California Institute for Research and Education; David R. Jacobs, PhD, of University of Minnesota; Deborah Levine, MD, PhD, of University of Michigan, Ann Arbor.
Funding: Please see the paper.
Disclosures: Yaffe reports serving on the Data Safety Monitoring Board for Eli Lilly and several National Institute on Aging sponsored studies, consultation services for Alpha Cognition, serving on the board of directors for Alector Inc., data and safety and monitoring services for Dominantly Inherited Alzheimer Network Trials Unit, and serving on the Beeson Scientific Advisory Board and the Global Council on Brain Health.
About this cognitive decline and inflammation research news
Author: Suzanne Leigh
Source: UCSF
Contact: Suzanne Leigh -UCSF
Image: The image is credited to Neuroscience News
Original Research: Closed access.
“Association of Changes in C-Reactive Protein Level Trajectories Through Early Adulthood With Cognitive Function at Midlife: The CARDIA Study” by Amber Bahorik et al. Neurology
Abstract
Association of Changes in C-Reactive Protein Level Trajectories Through Early Adulthood With Cognitive Function at Midlife: The CARDIA Study
Background and Objectives
Late-life inflammation has been linked to dementia risk and preclinical cognitive decline, but less is known about early adult inflammation and whether this could influence cognition in midlife. We aimed to identify inflammation levels through early adulthood and determine association of these trajectories with midlife cognition.
Methods
We used data from the Coronary Artery Risk Development in Young Adults study to identify inflammation trajectories (C-reactive protein [CRP] level
Six cognitive domains were evaluated from tests of verbal memory, processing speed, executive function, verbal and category fluency, and global cognition; poor cognitive performance was defined as a decline of ≥1 SD less than the mean on each domain. The primary outcome was poor cognitive performance. Logistic regression was used to adjust for demographics, smoking, alcohol use, physical activity, and APOE 4 status.
Results
Among 2,364 participants, the mean (SD) age was 50.2 (3.5) years; 55% were female, and 57% were White. Three CRP trajectories emerged over 18 years: lower stable (45%), moderate/increasing (16%), and consistently higher (39%). Compared with lower stable CRP, both consistently higher (adjusted odds ratio [aOR] 1.67, 95% CI 1.23–2.26) and moderately/increasing (aOR 2.04, 95% CI 1.40–2.96) CRP had higher odds of poor processing speed; consistently higher CRP additionally had higher odds of poor executive function (aOR 1.36, 95% CI 1.00–1.88).
For memory (moderately/increasing aOR 1.36, 95% CI 1.00–1.88; consistently higher aOR 1.18, 95% CI 0.90–1.54), letter fluency (moderately/increasing aOR 1.00, 95% CI 0.69–1.43; consistently higher aOR 1.05, 95% CI 0.80–1.39), category fluency (moderately/increasing aOR 1.16, 95% CI 0.82–1.63; consistently higher aOR 1.11, 95% CI 0.85–1.45), or global cognition (moderately/increasing aOR 1.16, 95% CI 0.82–1.63; consistently higher aOR 1.11, 95% CI 0.85–1.45), no association was observed.
Discussion
Consistently higher or moderate/increasing inflammation starting in early adulthood may lead to worse midlife executive function and processing speed. Study limitations include selection bias due to loss to follow-up and reliance on CRP as the only inflammatory marker. Inflammation is important for cognitive aging and may begin much earlier than previously known.