Stress attenuates the flexible updating of aversive value

Raio, Candace M.; Hartley, Catherine A.; Orederu, Temidayo; Li, Jian; Phelps, Elizabeth A.

doi:10.1073/pnas.1702565114

Cited by 66 publications

(90 citation statements)

References 47 publications

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“…Whilst the instrumental deficits on both the most salient (reward and punishment) and reward-only, but not punishment-only condition, as reported here, may at first seem surprising given the well-established role of serotonin in aversive processing (Cools et al 2008), this indeed aligns with the literature across species: the key marmoset studies on serotonin depletion and perseveration were conducted in the appetitive domain (Clarke et al 2004;Walker et al 2009 The deleterious effects of serotonin depletion and stress on reversal learning can be interpreted as a selective impairment in integrating new information about a change in reinforcement contingencies, needed to update the representation of aversive value appropriately (Raio et al 2017). These authors invoked the phenomenon of stress-induced dopamine release (Pruessner et al 2004), which may dampen negative prediction errors evoked by contingency reversal (Cools et al 2001).…”

Section: Discussionsupporting

confidence: 81%

“…Deficits in both domains were underscored by significant correlations showing that a greater extent of depletion, as assessed by plasma samples, was associated with more pronounced reversal impairments. Strikingly, the results align with data from neurotoxic serotonin depletion in experimental animals (Bari et al 2010;Clarke et al 2004Clarke et al , 2007Walker et al 2009), stress induction in humans (Raio et al 2017) That serotonin depletion impaired these fundamental learning processes pervasive in daily life highlights a failure mode that could lead to significant distress and impairment. The reversal deficits presented, furthermore, indicate how serotonergic dysfunction could impede the ability to engage in cognitive behavioural therapies (CBT).…”

Section: Discussionsupporting

confidence: 74%

“…), andSeymour et al (2012) found human ATD affected the appetitive but not aversive domain in a 4-choice probabilistic task on which computational modelling revealed enhanced perseveration.The Pavlovian reversal findings reported here resemble both the Pavlovian reversal learning impairment reported in OCD(Apergis-Schoute et al 2017) and what has been demonstrated in healthy volunteers under stress(Raio et al 2017). The reversal deficit in OCD, indexed by SCR on an identical paradigm, was explained by dysfunctional activity in the ventromedial prefrontal (vmPFC), which receives rich serotonergic innervation(Hornung 2010) Raio et al (2017),. meanwhile, used SCR and a similar design to that used here (but with neutral cues) and found that upon reversal, stress also attenuated the acquisition of threat responses to the newly threatening (previously safe) stimulus upon reversal, while leaving extinction learning to the previously threatening cue intact.…”

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confidence: 89%

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Serotonin depletion impairs both Pavlovian and instrumental reversal learning in healthy humans

Kanen

Apergis-Schoute

Yellowlees

et al. 2020

Preprint

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Serotonin is implicated in aversive processing and updating responses to changing environmental circumstances. Optimising behaviour to maximise reward and minimise punishment may require shifting strategies upon encountering new situations. Likewise, emotional reactions to threats are critical for survival yet must be modified as danger shifts from one source to another. Whilst numerous psychiatric disorders are characterised by behavioural and emotional inflexibility, few studies have examined the contribution of serotonin in humans. We modelled both processes in two independent experiments (N = 97), using instrumental and aversive Pavlovian reversal learning paradigms, respectively.Upon depleting the serotonin precursor tryptophan -in a double-blind randomised placebocontrolled design -healthy volunteers showed impairments in updating both behaviour and emotion to reflect changing contingencies. Reversal deficits in each domain, furthermore, were correlated with the extent of tryptophan depletion. These results translate findings in experimental animals to humans and have implications for the neurochemical basis of cognitive inflexibility.

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Section: Discussionsupporting

confidence: 81%

Section: Discussionsupporting

confidence: 74%

supporting

confidence: 89%

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Serotonin depletion impairs both Pavlovian and instrumental reversal learning in healthy humans

Kanen

Apergis-Schoute

Yellowlees

et al. 2020

Preprint

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“…Therefore, it is plausible that superior performance in the High CORT line may involve AMPAR-dependent mechanisms and/or several of the other mechanisms mentioned above. Conversely, in agreement with the findings that stress affects reversal learning (Graybeal et al, 2011) and that glucocorticoids modulate mechanisms involved in reversal (Bryce and Howland, 2015; Myers et al, 2014; Raio et al, 2017), our data suggest that the Low CORT responding line may exhibit altered neural activity in key brain regions involved in flexible behaviors. In fact, our former analyses of these rats indicate that the Low line exhibits lower basal activity in the ventral orbitofrontal cortex (OFC), prefrontal cortex (mPFC) and hippocampus as compared to the High line (Walker and Sandi, 2018).…”

Section: Discussionsupporting

confidence: 91%

Constitutive differences in glucocorticoid responsiveness are related to divergent spatial information processing abilities

Huzard

Vouros

Monari

et al. 2019

Preprint

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The stress response facilitates survival through adaptation and is intimately related to cognitive processes. The Morris water maze task probes spatial learning and memory in rodents and glucocorticoids (i.e. corticosterone in rats) have been suggested to elicit a facilitating action on memory formation. Moreover, the early aging period (around 16-18 months of age) is susceptible to stress- and glucocorticoid-mediated acceleration of cognitive decline. In this study, we tested three lines of rats selectively bred according to their individual differences in corticosterone responsiveness to repeated stress exposure during juvenility. We investigated whether endogenous differences in glucocorticoid responses influenced spatial learning, long-term memory and reversal learning abilities in a Morris water maze task at early aging. Additionally, we assessed the quality of the different swimming strategies of the rats. Our results indicate that rats with differential corticosterone responsiveness exhibit similar spatial learning abilities but different long-term memory retention and reversal learning. Specifically, the high corticosterone responding line had a better long-term spatial memory, while the low corticosterone responding line was impaired for both long-term retention and reversal learning. Our modeling analysis of performance strategies revealed further important line-related differences. Therefore, our findings support the view that individuals with high corticosterone responsiveness would form stronger long-term memories to navigate in stressful environments. Conversely, individuals with low corticosterone responsiveness would be impaired at different phases of spatial learning and memory.

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“…Computational modeling. In keeping with our prior computational model fitting approach (Raio et al, 2017), we fit and validated an associability model using individual subject SCRs. In the model, x n indicates the CS on trial n (CS ϩ or CS Ϫ ) and r n is the US (1 for US, 0 for no US).…”

Section: Methodsmentioning

confidence: 99%

Role of Human Ventromedial Prefrontal Cortex in Learning and Recall of Enhanced Extinction

Dunsmoor

Kroes

et al. 2019

J. Neurosci.

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Standard fear extinction relies on the ventromedial prefrontal cortex (vmPFC) to form a new memory given the omission of threat. Using fMRI in humans, we investigated whether replacing threat with novel neutral outcomes (instead of just omitting threat) facilitates extinction by engaging the vmPFC more effectively than standard extinction. Computational modeling of associability (indexing surprise strength and dynamically modulating learning rates) characterized skin conductance responses and vmPFC activity during noveltyfacilitated but not standard extinction. Subjects who showed faster within-session updating of associability during novelty-facilitated extinction also expressed better extinction retention the next day, as expressed through skin conductance responses. Finally, separable patterns of connectivity between the amygdala and ventral versus dorsal mPFC characterized retrieval of novelty-facilitated versus standard extinction memories, respectively. These results indicate that replacing threat with novel outcomes stimulates vmPFC involvement on extinction trials, leading to a more durable long-term extinction memory.

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Stress attenuates the flexible updating of aversive value

Cited by 66 publications

References 47 publications

Serotonin depletion impairs both Pavlovian and instrumental reversal learning in healthy humans

Serotonin depletion impairs both Pavlovian and instrumental reversal learning in healthy humans

Constitutive differences in glucocorticoid responsiveness are related to divergent spatial information processing abilities

Role of Human Ventromedial Prefrontal Cortex in Learning and Recall of Enhanced Extinction

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