20 research outputs found
Electrophysiological correlates of performance monitoring in middle and late adolescence
The ability to monitor and evaluate the consequences of ongoing behaviors and
coordinate behavioral adjustments seems to rely on networks including the anterior
cingulate cortex (ACC) and phasic changes in dopamine activity. Activity (and
presumably functional maturation) of the ACC may be indirectly measured using the
error-related negativity (ERN), an event-related potential (ERP) component that is
hypothesized to reflect activity of the automatic response monitoring system. To date, no
studies have examined the measurement reliability of the ERN as a trait-like measure of
response monitoring, its development in mid- and late- adolescence as well as its relation
to risk-taking and empathic ability, two traits linked to dopaminergic and ACC activity.
Utilizing a large sample of 15- and 18-year-old males, the present study examined the
test-retest reliability of the ERN, age-related changes in the ERN and other components
of the ERP associated with error monitoring (the Pe and CRN), and the relations of the
error-related ERP components to personality traits of risk propensity and empathy.
Results indicated good test-retest reliability of the ERN providing important validation of
the ERN as a stable and possibly trait-like electrophysiological correlate of performance
monitoring. Ofthe three components, only the ERN was of greater amplitude for the
older adolescents suggesting that its ACC network is functionally late to mature, due to
either structural or neurochemical changes with age. Finally, the ERN was smaller for
those with high risk propensity and low empathy, while other components associated with
error monitoring were not, which suggests that poor ACe function may be associated
with the desire to engage in risky behaviors and the ERN may be influenced by the extent
of individuals' concern with the outcome of events
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Individual Differences in Reinforcement Learning: Behavioral, Electrophysiological, and Neuroimaging Correlates
During reinforcement learning, phasic modulations of activity in midbrain dopamine neurons are conveyed to the dorsal anterior cingulate Cortex (dACC) and basal ganglia (BG) and serve to guide adaptive responding. While the animal literature supports a role for the dACC in integrating reward history over time, most human electrophysiological Studies of dACC function have focused on responses to single positive and negative outcomes. The present electrophysiological study investigated the role of the dACC in probabilistic reward learning in healthy subjects using a task that required integration of reinforcement history over time. We recorded the feedback-related negativity (FRN) to reward feedback in subjects who developed a response bias toward a more frequently rewarded ("rich") stimulus ("learners") versus subjects who did not ("non-learners"). Compared to non-learners, learners showed more positive (i.e., smaller) FRNs and greater dACC activation upon receiving reward for correct identification of the rich stimulus. In addition, dACC activation and a bias to select the rich Stimulus were positively correlated. The same participants also completed a monetary incentive delay (MID) task administered during functional magnetic resonance imaging. Compared to non-learners, learners displayed stronger BG responses to reward in the MID task. These findings raise the possibility that learners in the probabilistic reinforcement task were characterized by stronger dACC and BG responses to rewarding outcomes. Furthermore, these results highlight the importance of the dACC to probabilistic reward learning in humans.Psycholog
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Single Dose of a Dopamine Agonist Impairs Reinforcement Learning in Humans: Evidence from Event-related Potentials and Computational Modeling of Striatal-Cortical Function
Animal findings have highlighted the modulatory role of phasic dopamine (DA) signaling in incentive learning, particularly in the acquisition of reward-related behavior. In humans, these processes remain largely unknown. In a recent study, we demonstrated that a single low dose of a D2/D3 agonist (pramipexole) - assumed to activate DA autoreceptors and thus reduce phasic DA bursts - impaired reward learning in healthy subjects performing a probabilistic reward task. The purpose of this study was to extend these behavioral findings using event-related potentials and computational modeling. Compared with the placebo group, participants receiving pramipexole showed increased feedback-related negativity to probabilistic rewards and decreased activation in dorsal anterior cingulate regions previously implicated in integrating reinforcement history over time. Additionally, findings of blunted reward learning in participants receiving pramipexole were simulated by reduced presynaptic DA signaling in response to reward in a neural network model of striatal-cortical function. These preliminary findings offer important insights on the role of phasic DA signals on reinforcement learning in humans and provide initial evidence regarding the spatiotemporal dynamics of brain mechanisms underlying these processes.Psycholog
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Single Dose of a Dopamine Agonist Impairs Reinforcement Learning in Humans: Behavioral Evidence from a Laboratory-based Measure of Reward Responsiveness
Rationale. The dopaminergic system, particularly D2-like dopamine receptors, has been strongly implicated in reward processing. Animal studies have emphasized the role of phasic dopamine (DA) signaling in reward-related learning, but these processes remain largely unexplored in humans. Objectives. To evaluate the effect of a single, low dose of a D2/D3 agonist-pramipexole-on reinforcement learning in healthy adults. Based on prior evidence indicating that low doses of DA agonists decrease phasic DA release through autoreceptor stimulation, we hypothesized that 0.5 mg of pramipexole would impair reward learning due to presynaptic mechanisms. Materials and methods. Using a double-blind design, a single 0.5-mg dose of pramipexole or placebo was administered to 32 healthy volunteers, who performed a probabilistic reward task involving a differential reinforcement schedule as well as various control tasks. Results. As hypothesized, response bias toward the more frequently rewarded stimulus was impaired in the pramipexole group, even after adjusting for transient adverse effects. In addition, the pramipexole group showed reaction time and motor speed slowing and increased negative affect; however, when adverse physical side effects were considered, group differences in motor speed and negative affect disappeared. Conclusions. These findings show that a single low dose of pramipexole impaired the acquisition of reward-related behavior in healthy participants, and they are consistent with prior evidence suggesting that phasic DA signaling is required to reinforce actions leading to reward. The potential implications of the present findings to psychiatric conditions, including depression and impulse control disorders related to addiction, are discussed.Psycholog
Resting and reactive frontal brain electrical activity (EEG) among a non-clinical sample of socially anxious adults: Does concurrent depressive mood matter?
A number of studies have noted that the pattern of resting frontal brain electrical activity (EEG) is related to individual differences in affective style in healthy infants, children, and adults and some clinical populations when symptoms are reduced or in remission. We measured self-reported trait shyness and sociability, concurrent depressive mood, and frontal brain electrical activity (EEG) at rest and in anticipation of a speech task in a non-clinical sample of healthy young adults selected for high and low social anxiety. Although the patterns of resting and reactive frontal EEG asymmetry did not distinguish among individual differences in social anxiety, the pattern of resting frontal EEG asymmetry was related to trait shyness after controlling for concurrent depressive mood. Individuals who reported a higher degree of shyness were likely to exhibit greater relative right frontal EEG activity at rest. However, trait shyness was not related to frontal EEG asymmetry measured during the speech-preparation task, even after controlling for concurrent depressive mood. These findings replicate and extend prior work on resting frontal EEG asymmetry and individual differences in affective style in adults. Findings also highlight the importance of considering concurrent emotional states of participants when examining psychophysiological correlates of personality
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Enhanced Negative Feedback Responses in Remitted Depression
Major depressive disorder (MDD)is characterized by hypersensitivity to negative feedback that might involve frontocingulate dysfunction. MDD patients exhibit enhanced electrophysiological responses to negative internal (errors) and external (feedback) cues. Whether this dysfunction extends to remitted depressed (RD) individuals with a history of MDD is currently unknown. To address this issue, we examined the feedback-related negativity in RD and control participants using a probabilistic punishment learning task. Despite equivalent behavioral performance, RD participants showed larger feedback-related negativities to negative feedback relative to controls; group differences remained after accounting for residual anxiety and depressive symptoms. The present findings suggest that abnormal responses to negative feedback extend to samples at increased risk for depressive episodes in the absence of current symptoms.Psycholog
Developmental and individual differences in novelty and error detection in 10-year-old children and young adults /
Event-related potentials were recorded from 10-year-old children and young adults in
order to examine the developmental dififerences in two frontal lobe functions: detection of
novel stimuli during an auditory novelty oddball task, and error detection during a visual
flanker task. All participants showed a parietally-maximal P3 in response to auditory stimuli.
In children, novel stimuli generated higher P3 amplitudes at the frontal site compared with
target stimuli, whereas target stimuli generated higher P3 amplitudes at the parietal site
compared with novel stimuli. Adults, however, had higher P3 amplitude to novel tones
compared with target tones at each site. Children also had greater P3 amplitude at more
parietal sites than adults during the novelty oddball and flanker tasks. Furthermore, children
and adults did not show a significant reduction in P3 amplitude from the first to second novel
stimulus presentation. No age differences were found with respect to P3 latency to novel and
target stimuli. These findings suggest that the detection of novel and target stimuli is mature
in 10-year-olds.
Error trials typically elicit a negative ERP deflection (the ERN) with a frontal-central
scalp distribution that may reflect response monitoring. There is also evidence of a positive
ERP peak (the Pe) with a posterior scalp distribution which may reflect subjective
recognition of a response. Both children and adults showed an ERN and Pe maximal at
frontal-central sites. Children committed more errors, had smaller ERN across sites, and had
a larger Pe at the parietal site than adults. This suggests that response monitoring is still
immature in 10-year-olds whereas recognition of and emotional responses to errors may be
similar in children and adults