Role of interval timing in intertemporal choice: A behavioural and drift-diffusion model investigation

Value-based decision-making is of central interest in cognitive neuroscience and psychology, as well as in the context of neuropsychiatric disorders characterised by decision-making impairments. Studies examining (neuro-)computational mechanisms underlying choice behaviour typically focus on participants' decisions. However, there is increasing evidence that option valuation might also be reflected in motor response vigour and eye movements, implicit measures of subjective utility. To examine motor response vigour and visual fixation correlates of option valuation in intertemporal choice, we set up a task where the participants selected an option by pressing a grip force transducer, simultaneously tracking fixation shifts between options. As outlined in our preregistration (https://osf.io/k6jct), we used hierarchical Bayesian parameter estimation to model the choices assuming hyperbolic discounting, compared variants of the softmax and drift diffusion model, and assessed the relationship between response vigour and the estimated model parameters. The behavioural data were best explained by a drift diffusion model specifying a non-linear scaling of the drift rate by the subjective value differences. Replicating previous findings (Green et al., 1997; Wagner et al., 2020a), we found a magnitude effect for temporal discounting, such that higher rewards were discounted less. This magnitude effect was further reflected in response vigour, such that stronger forces were exerted in the high vs. the low magnitude condition. Bayesian hierarchical linear regression further revealed higher grip forces, faster response times and a lower number of fixation shifts for trials with higher subjective value differences. Our data suggest that subjective utility or implicit valuation is reflected in response vigour during intertemporal choice. Taking into account response vigour might thus provide deeper insight into decision-making, reward valuation and maladaptive changes in these processes, e.g. in the context of neuropsychiatric disorders.

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An adaptive drift-diffusion model of interval timing dynamics

Behavioural Processes ◽

10.1016/j.beproc.2013.02.003 ◽

2013 ◽

Vol 95 ◽

pp. 90-99 ◽

Cited By ~ 22

Author(s):

Andre Luzardo ◽

Elliot A. Ludvig ◽

François Rivest

Keyword(s):

Diffusion Model ◽

Interval Timing ◽

Drift Diffusion Model ◽

Drift Diffusion

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A drift–diffusion model of interval timing in the peak procedure

Journal of Mathematical Psychology ◽

10.1016/j.jmp.2016.10.002 ◽

2017 ◽

Vol 77 ◽

pp. 111-123 ◽

Cited By ~ 10

Author(s):

André Luzardo ◽

François Rivest ◽

Eduardo Alonso ◽

Elliot A. Ludvig

Keyword(s):

Diffusion Model ◽

Interval Timing ◽

Drift Diffusion Model ◽

Drift Diffusion ◽

Peak Procedure

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Dopamine and risky decision-making in pathological and problem gamblers

10.1101/805929 ◽

2019 ◽

Author(s):

Jan Peters ◽

Taylor Vega ◽

Dawn Weinstein ◽

Jennifer Mitchell ◽

Andrew Kayser

Keyword(s):

Decision Making ◽

Diffusion Model ◽

Gambling Disorder ◽

Risky Choice ◽

Drift Diffusion Model ◽

Drift Diffusion ◽

Problem Gamblers ◽

Cohen’S D ◽

Cohen's D

AbstractGambling disorder is a behavioral addiction that is associated with impairments in value-based decision-making such as increased temporal discounting and reduced risk-aversion. Dopamine regulates learning and decision-making by modulating information processing throughout fronto-striatal circuits. Although the role of alterations in dopamine neurotransmission in the etiology of gambling disorder is controversial, preliminary evidence suggests that specifically increasing frontal dopamine levels might improve cognitive functioning in pathological and problem gamblers. We therefore examined whether increasing frontal dopamine levels via the catechol-O-methyltransferase (COMT) inhibitor tolcapone would reduce risky choice in a group of pathological and problem gamblers (n=14) in a repeated-measures counter-balanced placebo-controlled double-blind study. Choice data were fit using hierarchical Bayesian parameter estimation and a modeling scheme that combined a risky choice model with the drift diffusion model to account for both choices and response time distributions. Model comparison revealed that the data were best accounted for by a variant of the drift diffusion model with a non-linear modulation of trial-wise drift rates by value differences, confirming recent findings. Contrary to our hypothesis, risk-taking was slightly increased under tolcapone vs. placebo (Cohen’s d = −.281). Examination of drug effects on diffusion model parameters revealed an increase in the value-dependency of the drift rate (Cohen’s d = .932) with a simultaneous reduction in the maximum drift rate (Cohen’s d = −1.84). These results add to previous work on the potential role of COMT inhibitors in behavioral addictions, and show no consistent beneficial effect of tolcapone on risky choice in gambling disorder. Modeling results add to mounting evidence for the applicability of diffusion models in value-based decision-making. Future work should focus on individual genetic, clinical and cognitive factors that might account for the heterogeneity in the effects of COMT inhibition.

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