Abstract
Background: The brain-derived neurotrophic factor (BDNF) protein has been shown to have a prominent role in neuron survival, growth, and function in experimental models, and the BDNF Val66Met polymorphism which regulates its expression has been linked to resilience toward the effects of aging on cognition. Cognitively stimulating activity is linked to both increased levels of BDNF in the brain, and protection against age-related cognitive decline. The aim of this study was to investigate the associations between serum BDNF levels, the BDNF Val66Met genotype, and components of cognitive reserve in early and mid-life, measured with the Lifetime of Experiences Questionnaire (LEQ).Methods: Serum BDNF levels were measured cross-sectionally in 156 participants from the Tasmanian Healthy Brain Project (THBP) cohort, a study examining the potential benefits of older adults engaging in a university-level education intervention. Multiple linear regression was used to estimate serum BDNF’s association with age, education, gender, BDNF Val66Met genotype, later-life university-level study, and cognitively stimulating activities measured by the LEQ.Results: Serum BDNF in older adults was associated with early life education and training, increasing 0.007 log(pg/ml) [95%CI 0.001, 0.012] per unit on the LEQ subscale. Conversely, education and training in mid-life were associated with a −0.007 log(pg/ml) [−0.012, −0.001] decrease per unit on the LEQ subscale. Serum BDNF decreased with age (−0.008 log(pg/ml) [−0.015, −0.001] per year), and male gender (−0.109 log(pg/ml) [−0.203, −0.015]), but mean differences between the BDNF Val66Met polymorphisms were not significant (p = 0.066). All effect sizes were small, with mid-life education and training having the largest effect size ( = 0.044).Conclusion: Education in both early and mid-life explained small but significant amounts of variance in serum BDNF levels, more than age or gender. These effects were opposed and independent, suggesting that education at different stages of life may be associated with different cognitive and neural demands. Education at different stages of life may be important covariates when estimating associations between other exposures and serum BDNF.
Highlights
A of evidence suggests an individual’s risk of developing dementia is influenced by genetic and environmental factors, and their interactions (Lourida et al, 2019)
Higher serum brain-derived neurotrophic factor (BDNF) levels have been suggested to protect against dementia occurrence (Weinstein et al, 2014), they may represent an important mediator of the beneficial effects of cognitively stimulating activities on cognitive reserve and dementia risk
To account for Tasmanian Healthy Brain Project (THBP) participant’s engagement with cognitively stimulating activities at different stages across the lifespan, the cognitive reserve was treated as individual subscales from; university study, premorbid intelligence quotient [Weschler Test of Adult Reading (WTAR), Full-Scale IQ (FSIQ)], and lifetime cognitive stimulation [Lifetime Experiences Questionnaire (LEQ)]
Summary
A of evidence suggests an individual’s risk of developing dementia is influenced by genetic and environmental factors, and their interactions (Lourida et al, 2019). One environmental factor which has been strongly linked to dementia risk is early life education, with lower levels of education conferring an increased risk of dementia (Livingston et al, 2020) and cognitive stimulation suggested to improve resilience to dementia. Conclusion: Education in both early and mid-life explained small but significant amounts of variance in serum BDNF levels, more than age or gender These effects were opposed and independent, suggesting that education at different stages of life may be associated with different cognitive and neural demands.
Sign-in/Register to view highlights & summary Sign-in/Register to access full text options 
Free) 
Talk to us
Join us for a 30 min session where you can share your feedback and ask us any queries you have
Schedule a call
