92 research outputs found
Age Differences in Striatal Delay Sensitivity during Intertemporal Choice in Healthy Adults
Intertemporal choices are a ubiquitous class of decisions that involve selecting between outcomes available at different times in the future. We investigated the neural systems supporting intertemporal decisions in healthy younger and older adults. Using functional neuroimaging, we find that aging is associated with a shift in the brain areas that respond to delayed rewards. Although we replicate findings that brain regions associated with the mesolimbic dopamine system respond preferentially to immediate rewards, we find a separate region in the ventral striatum with very modest time dependence in older adults. Activation in this striatal region was relatively insensitive to delay in older but not younger adults. Since the dopamine system is believed to support associative learning about future rewards over time, our observed transfer of function may be due to greater experience with delayed rewards as people age. Identifying differences in the neural systems underlying these decisions may contribute to a more comprehensive model of age-related change in intertemporal choice
Gain and Loss Learning Differentially Contribute to Life Financial Outcomes
Emerging findings imply that distinct neurobehavioral systems process gains and losses. This study investigated whether individual differences in gain learning and loss learning might contribute to different life financial outcomes (i.e., assets versus debt). In a community sample of healthy adults (n = 75), rapid learners had smaller debt-to-asset ratios overall. More specific analyses, however, revealed that those who learned rapidly about gains had more assets, while those who learned rapidly about losses had less debt. These distinct associations remained strong even after controlling for potential cognitive (e.g., intelligence, memory, and risk preferences) and socioeconomic (e.g., age, sex, ethnicity, income, education) confounds. Self-reported measures of assets and debt were additionally validated with credit report data in a subset of subjects. These findings support the notion that different gain and loss learning systems may exert a cumulative influence on distinct life financial outcomes
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Individual Differences in Dopamine Are Associated with Reward Discounting in Clinical Groups But Not in Healthy Adults.
Some people are more willing to make immediate, risky, or costly reward-focused choices than others, which has been hypothesized to be associated with individual differences in dopamine (DA) function. In two studies using PET imaging, one empirical (Study 1: N = 144 males and females across 3 samples) and one meta-analytic (Study 2: N = 307 across 12 samples), we sought to characterize associations between individual differences in DA and time, probability, and physical effort discounting in human adults. Study 1 demonstrated that individual differences in DA D2-like receptors were not associated with time or probability discounting of monetary rewards in healthy humans, and associations with physical effort discounting were inconsistent across adults of different ages. Meta-analytic results for temporal discounting corroborated our empirical finding for minimal effect of DA measures on discounting in healthy individuals but suggested that associations between individual differences in DA and reward discounting depend on clinical features. Addictions were characterized by negative correlations between DA and discounting, but other clinical conditions, such as Parkinson's disease, obesity, and attention-deficit/hyperactivity disorder, were characterized by positive correlations between DA and discounting. Together, the results suggest that trait differences in discounting in healthy adults do not appear to be strongly associated with individual differences in D2-like receptors. The difference in meta-analytic correlation effects between healthy controls and individuals with psychopathology suggests that individual difference findings related to DA and reward discounting in clinical samples may not be reliably generalized to healthy controls, and vice versa.SIGNIFICANCE STATEMENT Decisions to forgo large rewards for smaller ones due to increasing time delays, uncertainty, or physical effort have been linked to differences in dopamine (DA) function, which is disrupted in some forms of psychopathology. It remains unclear whether alterations in DA function associated with psychopathology also extend to explaining associations between DA function and decision making in healthy individuals. We show that individual differences in DA D2 receptor availability are not consistently related to monetary discounting of time, probability, or physical effort in healthy individuals across a broad age range. By contrast, we suggest that psychopathology accounts for observed inconsistencies in the relationship between measures of DA function and reward discounting behavior
Correspondence: Are Cognitive Functions Localizable? Colin Camerer et al. versus Marieke van Rooij and John G. Holden
The Fall 2011 issue of this journal published a
two-paper section on “Neuroeconomics.” One
paper, by Ernst Fehr and Antonio Rangel, clearly
and concisely summarized a small part of the fast-growing
literature. The second paper, “It’s about
Space, It’s about Time, Neuroeconomics, and the
Brain Sublime,” by Marieke van Rooij and Guy Van
Orden, is beautifully written and enjoyable to read,
but misleading in many critical ways. A number
of economists and neuroscientists working at the
intersection of the two fields shared our reaction
and have signed this letter, as shown below. Some of
the paper’s descriptions of empirical findings and
methods in neuroeconomics are incomplete, badly
out of date, or flatly wrong. In studies the authors
describe in detail, their skeptical interpretations
have often been refuted by published data, old and
new, that they overlook
Foraging, exploration, or search? On the (lack of) convergent validity between three behavioral paradigms
Recently it has been suggested that individual humans and other animals possess different levels of a general tendency to explore or exploit that may influence behavior in different contexts. In the present work, we investigated whether individual differences in this general tendency to explore (exploit) can be captured across three behavioral paradigms that involve exploration–exploitation trade-offs: A foraging task involving sequential search for fish in several ponds, a multiarmed bandit task involving repeatedly choosing from a set of options, and a sequential choice task involving choosing a candidate from a pool of applicants. Two hundred and sixty-one participants completed two versions of each of the three tasks. Structural equation modeling revealed that there was no single, general factor underlying exploration behavior in all tasks, even though individual differences in exploration were stable across the two versions of the same task. The results suggest that task-specific factors influence individual levels of exploration. This finding causes difficulties in the enterprise of measuring general exploration tendencies using single behavioral paradigms and suggests that more work is needed to understand how general exploration tendencies and task-specific characteristics translate into exploratory behavior in different contexts
Serotonergic genotypes, neuroticism, and financial choices.
Life financial outcomes carry a significant heritable component, but the mechanisms by which genes influence financial choices remain unclear. Focusing on a polymorphism in the promoter region of the serotonin transporter gene (5-HTTLPR), we found that individuals possessing the short allele of this gene invested less in equities, were less engaged in actively making investment decisions, and had fewer credit lines. Short allele carriers also showed higher levels of the personality trait neuroticism, despite not differing from others with respect to cognitive skills, education, or wealth. Mediation analysis suggested that the presence of the 5-HTTLPR short allele decreased real life measures of financial risk taking through its influence on neuroticism. These findings show that 5-HTTLPR short allele carriers avoid risky and complex financial choices due to negative emotional reactions, and have implications for understanding and managing individual differences in financial choice
The fossil record of primate brain evolution (James Arthur lecture on the evolution of the human brain, no. 49, 1979).
27 p. : ill. ; 23 cm. Includes bibliographical references (p. 25-27)
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