Abstract

Introduction

Decline in processing speed, memory, and executive function is a relatively widespread characteristic of aging (Li et al., 2001; Bishop et al., 2010; Silver et al., 2011; El Haj and Allain, 2012; Singh-Manoux et al., 2012; Woodard et al., 2012). Several neural mechanisms thought to support these cognitive processes become particularly vulnerable during the aging process (Burke and Barnes, 2006). For instance, brain-derived neurotrophic factor (BDNF) levels tend to decrease progressively with age (Lommatzsch et al., 2005; Ziegenhorn et al., 2007; Driscoll et al., 2012) and correlate with age-related reductions in hippocampal volume (Erickson et al., 2010a). BDNF facilitates neural repair (Yang et al., 2014), induces long-term potentiation (Diógenes et al., 2011), enhances learning and memory (Pang and Lu, 2004; Bekinschtein et al., 2014), and promotes synaptic plasticity and neurogenesis (Oliff et al., 1998; Lu, 2003; Vaynman et al., 2004). The beneficial effects of BDNF on brain health and cognition may be especially relevant for older adults, who are susceptible to physiological changes that interfere with neural processes and cognitive function. For instance, marked increases in blood pressure and inflammatory load occur in older adulthood, both of which have been independently linked to dementia risk and decline in cognitive function (Schmidt et al., 2002; Singh and Newman, 2011). Thus, there is an increased presence of factors that compromise cognitive function in older adults, with a contemporaneous decrease in known mechanisms that support advantageous brain and cognitive health. Therefore, efforts to increase BDNF, particularly in older aged individuals, could play an important role in the preservation of cognitive function.

Fortunately, exercise may be an effective approach to preserve and improve cognitive function and brain health in late adulthood. For example, randomized clinical trials have found that moderate-intensity exercise improves memory and executive function (Kramer et al., 1999a; Colcombe and Kramer, 2003; Smith et al., 2010) increases prefrontal cortex (Colcombe et al., 2006) and hippocampal volume (Erickson et al., 2011), and influences brain network connectivity (Voss et al., 2010a). Cross-sectional and epidemiological studies have supported these results and demonstrate that higher fitness levels and greater amounts of physical activity are associated with greater gray matter volumes (Erickson et al., 2010b; Weinstein et al., 2012; Benedict et al., 2013), white matter integrity (Gow et al., 2012; Gons et al., 2013; Tian et al., 2014), reduced brain atrophy rates (Gow et al., 2012; Smith et al., 2014), and reduced risk of cognitive impairment and dementia (Podewils et al., 2005; Larson et al., 2006; Sofi et al., 2011). Yet, the mechanisms by which exercise improves or maintains brain health in humans remain poorly understood, but likely include changes in inflammation, insulin resistance, as well as central changes in serotonin, dopamine, or other neurotransmitters.

Increased expression of BDNF may be another mechanism by which exercise positively influences cognitive and brain function. For example, in rodents, exercise increases BDNF expression in the striatum (Marais et al., 2009), hippocampus (Aguiar et al., 2011), and cortex (Neeper et al., 1996) and an exercise-induced up-regulation of BDNF, along with its receptor tyrosine kinase (Li et al., 2008), mediates the effects of exercise on cognition (Gómez-Pinilla et al., 2002; Vaynman et al., 2004; Van Praag et al., 2005; Stranahan et al., 2009; Creer et al., 2010; Bechara and Kelly, 2013). Unfortunately in humans the effect of exercise on serum BDNF is more equivocal (Zoladz and Pilc, 2010). Acute bouts of exercise increase serum BDNF levels, which, in turn, are associated with improvements in cognitive performance (Knaepen et al., 2010; Ströhle et al., 2010; Heyman et al., 2012; Coelho et al., 2013). However, more chronic and longer-term exercise programs have not reliably demonstrated increases in BDNF levels (Baker et al., 2010; Erickson et al., 2011; Ruscheweyh et al., 2011). Despite these discouraging effects of exercise interventions, exercise-induced changes in hippocampal volume (Erickson et al., 2011) and brain connectivity (Voss et al., 2013) were correlated with percent change in serum BDNF levels. These findings suggest that serum BDNF levels may be an important biomarker for brain and cognitive health, but whether BDNF mediates the positive effects of exercise on cognitive performance remains a matter of speculation.

Here, we examine whether exercise-induced changes in serum BDNF mediates the effect of a randomized exercise intervention on executive function. Specifically, we assessed effects on task-switch performance, a cognitive task largely susceptible to age-related shifts in performance speed and accuracy (Salthouse et al., 1998; Kray and Lindenberger, 2000; Cepeda et al., 2001; Jimura and Braver, 2010; Gazes et al., 2012). This task is considered a measure of executive control and is supported primarily by the prefrontal and parietal cortices (Sohn et al., 2000; Braver et al., 2003; Aron et al., 2004; Gold et al., 2010), regions that experience preferential degeneration with advancing age (Sowell et al., 2003; Salat et al., 2005; Driscoll et al., 2009). Because BDNF levels decline with age (Lommatzsch et al., 2005; Burke and Barnes, 2006; Ziegenhorn et al., 2007), and is found in cortical regions that likely support task-switch performance (Podewils et al., 2005; Aguiar et al., 2011; Diógenes et al., 2011), we reasoned that age might be an important moderator of the effects of exercise on BDNF and task-switch performance.

Prior studies examining the effects of exercise on serum BDNF have used age as a covariate rather than modeling age as an interaction term. Yet, several studies and meta-analyses suggest that the positive effects of exercise on cognitive performance may be magnified at older ages (Etnier et al., 2007; Smith et al., 2010) while others have found that age-related losses in gray matter volume and n-acetylaspartate levels were mitigated by higher fitness levels (Colcombe et al., 2003; Erickson et al., 2012). These and other studies (Adlard et al., 2005; Knaepen et al., 2010) suggest that age might be moderating an effect of exercise on serum BDNF levels.

The current study examined the effects of a 12-month randomized exercise intervention on serum BDNF and task-switching performance in older adults. We predicted that exercise-induced changes in serum BDNF would mediate the effects of the exercise intervention on task-switch performance. However, we also predicted that age would moderate the effect of the intervention on BDNF levels, such that the oldest adults in the exercise group would show greater increases in BDNF than their younger counterparts.

Method

Cognitive assessment

The task-switching paradigm is frequently used to assess executive processes (Kramer et al., 1999a; Kray and Lindenberger, 2000; Gratton et al., 2009; Gold et al., 2010; Jimura and Braver, 2010), including cognitive flexibility and inhibition (Verstynen et al., 2012). The task-switch paradigm was administered as part of a larger battery of tasks, but was selected for the present study because (1) it assesses executive functioning and (2) our previous studies have shown that this task is sensitive to exercise interventions (Kramer et al., 1999a,b). Therefore, we selected this task because it met criteria for testing mediation.

As described in Voss et al. (2010a), participants utilized color-based cues to determine whether they were to judge whether a number was odd or even, or whether it was low or high (i.e., smaller or larger than 5). The numbers were presented individually for 1500 ms against a pink or blue background. If the background was blue, participants had to determine whether the number was high (“X” key) or low (“Z” key). If the background was pink, participants were to report whether the number was odd (“N” key) or even (“M” key). In both cases, participants were asked to answer as quickly as possible (Voss et al., 2010a). Participants completed a practice block followed by two blocks of individually presented tasks, one block consisted of only the “high or low” task, and the other consisted of only the “odd or even” task. This was followed by a switching block, which included 120 trials with the task in each trial chosen randomly. In this block, some trials were repeated, referred to here as “repeat trials,” and some trials switched between the two conditions, referred to here as “switch trials” (see Figure ​Figure11 for task depiction).

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Figure 1

Display of the task-switch paradigm. Participants were instructed to respond to a number between 1 and 9 (except for 5) that appeared centrally located on the computer screen. The background color (blue/pink) cued them as to the task they would do (Pink: even/odd; Blue: higher/lower than 5). In the single task condition participants were presented with blocks of a single task whereas in the mixed condition the two conditions were randomly presented.

Accuracy (% correct) and reaction time (RT) served as indices of performance on the task-switch test. Accuracy (% correct) and time (RT) was recorded separately for single trials, repeat trials within the mixed block, and switch trials within the mixed block. Local switch cost, the difference between repeat trials (when the preceding trial involved the same task) and switch trials (when the preceding trial involved a different task) was calculated for both RT and accuracy (Verstynen et al., 2012). Additionally, global switch cost, the difference between switch trials and single task trials, was calculated for RT and accuracy.

Statistical analysis

All variables were tested for normality and skew. To assess whether age was inversely associated with serum BDNF, we conducted a multivariable linear regression analysis. BDNF genotype was included as a covariate in the model to adjust for effects of the val66met polymorphism on BDNF serum concentrations.

To examine whether the effect of exercise group (walking; stretching) on serum BDNF varied as a function of age, multivariable linear regression was employed using the bootstrap method with 10,000 resampling iterations. Therefore, main effects and interaction effects were estimated from the resampled data repeatedly drawn from the original dataset with replacement. Within the regression model, pre-intervention serum BDNF was included as a covariate to account for any group-level differences in serum BDNF at baseline. Gender and the BDNF val66met polymorphism were also adjusted for in the model. Exercise group and age were entered as predictor terms to determine whether age and group independently predicted change in serum BDNF. We also included an age × group interaction in order to test whether age moderated the effect of exercise group on change in serum BDNF.

We also predicted that age would moderate the association between exercise group and cognitive performance post-intervention. To test this hypothesis, we used multivariable linear regression adjusting for gender, years of education, baseline serum BDNF, the BDNF val66met polymorphism, and baseline cognitive performance. Thus, rather than modeling within-subject changes in cognitive performance, we assessed group-level differences in performance post-intervention, accounting for individual differences in performance at baseline. Again, bootstrapping was applied to the regression model, using 10,000 iterations. Also entered was group, age as a continuous variable, and their interaction product. A statistical threshold of p < 0.05 was used to determine significance for the linear regression analyses. Significant interactions revealed by the linear regression analyses were then subjected to repeated measures analysis of variance tests to assess within-subject changes from pre to post-intervention.

Finally, conditional process modeling was used to examine the conditional nature by which exercise group predicts cognitive function following the 1-year intervention. Using this procedure, we examined whether BDNF serum levels mediated the relationship between exercise group and cognitive performance, and whether the indirect effect of exercise group on cognitive performance through serum BDNF varied as a function of age. This technique estimates the mediating effect of serum BDNF on the relationship between exercise group and task-switch performance, while accounting for moderating effects of age on (1) the effect of exercise group on serum BDNF and (2) the direct effect of exercise group on task-switch performance. The model format and analyses were conducted using the PROCESS macro by Hayes (2013) in SPSS. This method provided an estimation of both the direct and indirect pathways, resulting in the calculation of 95% confidence intervals (CI) for both direct and indirect effects (see Figure ​Figure22 for model depiction). The regression coefficients are displayed in unstandardized form, as the bootstrapped CI's correspond to the unstandardized effects rather than the standardized effects. Mediation results are considered significant if the CI's do not contain 0.

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Figure 2

Moderated mediation model. (A) Moderation Model: Effect of exercise group on BDNF serum levels as a function of age. (B) Mediation Model: Effect of exercise group on Task-Switch accuracy cost as a function of BDNF serum levels. Note: Solid arrow indicates direct pathway; Dashed arrow indicates indirect pathway. (C) Moderated Mediation Model: Mediating effect of BDNF serum levels on the effect of exercise group on Task-Switch accuracy cost as a function on age. Note: Solid arrow indicates moderation; Dashed arrow indicates mediation.

Results

Age moderates the effect of exercise on change in serum BDNF

The BDNF val66met polymorphism was not related to serum BDNF at baseline (r = 0.018; p = 0.868). Nonetheless, in the regression analyses described below we continued to control for BDNF val66met variation because several prior studies have indicated a small, but significant, relation between serum BDNF and the BDNF val66met polymorphism (Lang et al., 2009). We also found that females had significantly higher levels of serum BDNF at baseline in this sample (r = 0.266; p = 0.010) and therefore included gender as a covariate in the analyses below. Consistent with our hypothesis, older ages were associated with lower serum BDNF levels prior to the start of the intervention (t = −3.501; p = 0.001), after controlling for gender and the BDNF val66met polymorphism.

Collapsed across the intervention and control groups, age did not predict change in serum BDNF over the 1-year period (B = −77.69; p = 0.489). Similarly, holding age constant, there was not a main effect of exercise group on change in serum BDNF following the intervention, although the association was trending (B = 2652.27; p = 0.084). However, the lack of main effects was qualified by a significant interaction between age and exercise group on change in serum BDNF (B = 471.95; p = 0.036) (see Table ​Table3).3). Specifically, across the 1-year intervention, the stretching and toning group showed a decline in BDNF levels for the oldest individuals. In contrast, there was a positive linear relationship between age and serum BDNF in the walking group, indicating that older aged individuals experienced the greatest increase in BDNF following 1-year of moderate intensity walking exercise (see Figure ​Figure3B3B).

Table 3

Age moderates effect of exercise group on BDNF serum levels at post-intervention.

	B	SE	p	LLCI	ULCI
COVARIATES
Baseline serum BDNF	0.473**	0.109	0.0001	0.256	0.684
BDNF genotype	1152.29	2055.91	0.560	−2730.59	5415.26
Gender	1137.57	1834.59	0.535	−2555.65	4599.24
MAIN EFFECTS
Age	−77.69	112.27	0.490	−303.22	142.03
Exercise group	2652.27	1472.59	0.078	−373.40	5429.23
INTERACTION
Exercise group × Age	471.95*	1.735	0.039	26.261	919.647

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Age as moderator of the effect of exercise group on serum BDNF post-intervention. Coefficients are unstandardized B-values calculated from bootstrap permutation of 10,000 iterations.

LLCI, lower-level confidence interval; ULCI, upper-level confidence interval.

^*p < 0.05;

^**p < 0.01.

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Figure 3

Moderating effect of age (stratified). Note: Effects of exercise on serum BDNF as a function of age. Age stratified using a median split. (A) Serum BDNF decreases following the intervention in the control group among adults >65 years. (B) Serum BDNF increases following 1 year of walking exercise, specifically for adults aged >65 years.

For further exploration of this interaction, we used repeated measures analysis of variance and divided the sample into higher and lower aged individuals using the median value for age (Md age = 65). Serum BDNF at baseline and serum BDNF post-intervention were entered as the within subjects factor, age and exercise group were entered as between subjects factors, and BDNF genotype and gender were entered as covariates. Consistent with the results from the regression, participation in the walking group offset an age-related reduction in BDNF levels (F = 5.45; p = 0.022; η²_p = 0.060) (see Figure ​Figure3).3). In particular, 12 months of moderate intensity walking exercise increased serum BDNF levels among adults older than 65 years of age, while similarly aged individuals in the non-aerobic condition showed a decrease in serum BDNF over the 12-month intervention period.

BDNF mediates effect of exercise on task-switch performance as a function of age

The prior analyses demonstrated that the effect of exercise group on BDNF serum levels and task-switch performance varied as a function of age. Specifically, relative to the non-aerobic control condition, 12 months of moderate intensity aerobic exercise led to an increase in serum BDNF and an improvement in task performance (lower cost on global accuracy) that varied with age, with the oldest individuals showing the greatest benefits. Next, we tested whether serum BDNF mediates the association between exercise group and change in global accuracy cost following the 1-year intervention. Additionally, due to the robust age effects observed, a moderated mediation conditional processes model was used to examine whether serum BDNF explained the relation between exercise group and task-switch performance as a function of age. Thus, we first examined whether serum BDNF mediated the relation between exercise group and global accuracy cost. Then, we assessed whether the mediating effect of serum BDNF varied as a function of age. For these analyses, we focused only on the task variables that showed a significant age × group interaction effect (i.e., global accuracy cost). Since gender, education, and the BDNF val66met polymorphism did not significantly modify any of the above outcomes, they were removed from subsequent mediation models.

Mediation analyses revealed that there was not a direct effect of exercise group on global accuracy cost, after accounting for baseline serum BDNF and baseline global accuracy cost [B = 4.541; p = 0.160; CI(SE) −1.831; 10.912 (3.203)]. In contrast, there was a significant indirect effect of exercise group on global accuracy cost through serum BDNF [B = 1.317; CI(SE).058; 4.66 (1.007)]. Specifically, participants in the walking group scored, on average, 1.36 percent better on global accuracy cost, which was mediated by exercise-induced changes in serum BDNF levels. The average global accuracy cost was negative (−7.96%) indicating a smaller performance deficit between single and switch trials. Thus, 1 year of moderate-intensity aerobic exercise increased levels of serum BDNF, which, in turn, led to a decrease in cost performance.

Further, the conditional process analysis showed that there was a conditional indirect effect of exercise group on global accuracy cost through BDNF serum that differed by age [B = 0.168; CI(SE).009; 0.567 (0.129)] (see Table ​Table5).5). Further inspection revealed that serum BDNF levels mediated the relationship between exercise group and task-switch performance specifically for older aged individuals (see Figure ​Figure44).

Table 5

Moderated mediation model of effects of exercise group on global accuracy cost.

	B	SE	p	LLCI	ULCI
COVARIATES
Pre-intervention BDNF	0.0001	0.0002	0.584	−0.0003	0.0005
Baseline global accuracy cost	0.148*	0.062	0.020	0.024	0.271
MODERATED MEDIATION INDIRECT EFFECT
Post-intervention BDNF	0.168*	0.129		0.008	0.568
Effect at 10% Age (60 years)	−0.130	0.957		−2.108	1.868
Effect at 25% Age (63 years)	0.373	0.807		−0.761	2.662
Effect at 50% Age (65 years)	0.79	0.799		−0.263	3.162
Effect at 75% Age (71 years)	1.714*	1.183		0.260	5.382
Effect at 90% Age (76 years)	2.553*	1.716		0.390	7.807

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Moderated mediation model displaying BDNF as mediator of the effect of exercise group on post-intervention global accuracy cost (% correct) as a function of age. Includes overall effect and indirect effect of serum BDNF at different ages (stratified into quintiles).

^*p < 0.05—based on confidence interval.

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Figure 4

Mediating effect of BDNF within model, as a function of age. Note: Moderated mediation conditional indirect effect. Values of the y-axis are the unstandardized mediating effects (coefficients) of BDNF on the relationship between exercise group and task switch accuracy cost. Bars indicate age quintiles (10th, 25th, 50th, 75th, and 90th percentiles) on the x-axis. Sample distribution is as follows: Age <60: n = 13; 61–63: n = 21; 64–65; n = 12; 66–71: n = 23; 71–76: n = 16; >77: n = 7.

While the above analyses included age as a continuous predictor, to determine the age at which effects of BDNF mediated task switch accuracy cost, age was divided into quintiles (10th, 25th, 50th, 75th, and 90th percentiles). Effects were then calculated for each of these percentiles of age (60, 63, 65, 71, and 76 years), revealing that serum BDNF mediated the relationship between exercise group and task switch accuracy cost only among participants whose ages were in the 75th [B = 1.714; CI(SE) 0.260; 5.382 (1.183)] and 90th percentiles [B = 2.553; CI(SE) 0.390; 7.807 (1.716)], or 71 years of age and older. Thus, changes in serum BDNF mediated the relationship between exercise group and task performance, specifically for participants aged 71 years and older.

Discussion

In line with our hypotheses, changes in serum BDNF mediated the effect of the exercise intervention on task-switch performance. Interestingly, this effect varied as a function of age such that only individuals older than 71 years of age showed a significant mediating effect of BDNF on task-switch performance. Of note, this relationship is significant in a regression model using baseline task-switch performance as a covariate and when examining change in a RM-ANOVA analysis. These results indicate that moderate-intensity physical activity, such as walking, may be more beneficial to both BDNF and task-switching performance for adults over the age of 70 than younger individuals.

Similar to previous research (Ziegenhorn et al., 2007; Flöel et al., 2010), our results demonstrate that older age was associated with lower BDNF serum levels. However, this relationship was not present after the 1-year intervention for the walking exercise group. Exercise increased BDNF levels, but age moderated this relationship such that older adults in the walking group showed increases in BDNF that their younger exercising group members, nor their stretching control counterparts, displayed. This moderating effect of age may account for heterogeneity in the literature that report negligible associations between longer durations of exercise and BDNF levels in middle-aged adults and in samples with a limited age range (Schulz et al., 2004; Schiffer et al., 2009).

Of particular interest, we found evidence that serum BDNF mediated the association between a 12-month exercise intervention and improvements in executive function, but find that this mediating effect is dependent on the age of the sample. Rodent studies have also reported that BDNF mediates the effects of exercise on cognition and related brain pathways (Van Hoomissen et al., 2004; Vaynman et al., 2004; Hopkins and Bucci, 2010; Gómez-Pinilla and Feng, 2012). Yet, the current study is the first to demonstrate this effect in humans through a randomized controlled trial, and including both serum BDNF and BDNF genotype. What makes the current analyses unique is that the mediating effect of BDNF on cognition is independent of BDNF genotype, and present only in adults over the age of 70. These results highlight that age-related decreases in serum BDNF may be successfully mitigated by participation in exercise and that this might be a critical mechanism by which exercise improves executive function in late adulthood.

Our results also demonstrate that BDNF mediated the effect of exercise on task-switch accuracy cost, but not on response time, in adults aged 70 years or older. Accuracy on the task-switch paradigm is often interpreted as a measure of executive function ability to execute the task demands, while response times are interpreted as a measure of cognitive control, processing speed or efficiency (Hughes et al., 2013). Thus, our results demonstrate that the effects of exercise on the ability to execute the demands of a challenging task that taps into executive functions are mediated by BDNF in adults over the age of 70. We can only speculate as to the reason for the non-significant effects on response times. One possibility is that there are selective effects of BDNF on the neural correlates that support accuracy verses response times (Hughes et al., 2013). Specifically, BDNF may be mediating the effect of exercise on the prefrontal and parietal regions that support executive function (Jimura et al., 2014) and the “top-down” processing required for task-switch accuracy (Phillips et al., 2013), and not the striatum or regions which are associated with processing speed or response time outcomes (Jimura et al., 2014). Still, our results suggest that the modification in the level of serum BDNF is an important pathway by which exercise influences executive function for adults over 70 years of age.

Despite the strengths of our study, there remain several important limitations. First, analyses and interpretation of the results are based on serum BDNF levels, rather than BDNF directly from brain tissue. Importantly, rodent studies have found significant correlations between cortical BDNF and circulating BDNF levels (Karege et al., 2002), despite controversy on the validity of serum BDNF as a proxy for cortical concentrations (Knaepen et al., 2010). Thus, we believe that this is an acceptable limitation given the obvious challenges of obtaining brain tissue from human subjects. Additionally, while the sample size of each intervention group is similar-to or larger-than previous randomized clinical trials, the statistical models employed in the current analyses limit degrees of freedom and require a large sample to detect effects. It is possible that a larger sample would strengthen current findings or reveal effects in younger ages. Additionally, the current sample was mostly female with little representation of racial minorities, preventing generalization to a population outside of female Caucasians. Finally, our sample was relatively homogeneous without outward signs of cognitive impairment. Therefore, a more varied sample with different demographic characteristics and cognitive abilities may find different results than those described here.

The current findings indicate that adults over the age of 70 may gain the most from aerobic exercise in terms of both serum BDNF and task-switch performance. Indeed, the current sample shows no significant difference in BDNF serum levels or task switch performance at follow-up between the control and exercise intervention groups, however when examined as a function of age, BDNF levels significantly mediate the effect of exercise group on improvements in executive function. The results from this study do not preclude positive effects of exercise on other cognitive domains, other age ranges, other populations, or other putative mechanistic pathways (i.e., inflammatory). These findings highlight the importance of considering both age and BDNF when designing exercise interventions and interpreting the mechanism by which exercise improves cognitive performance, particularly in the elderly.

References