The effect of intranasal oxytocin treatment on conditioned fear extinction and recall in a healthy human sample

Acheson, Dean T.; Feifel, David; Wilde, Sofieke de; McKinney, R. Anne; Lohr, James B.; Risbrough, Victoria B.

doi:10.1007/s00213-013-3099-4

Cited by 124 publications

(110 citation statements)

References 45 publications

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“…To test the effects of oxytocin on extinction, we employed a common 2-day protocol; on the first day, fear conditioning was followed by drug treatment and subsequent extinction training trials, with the fear recall test 24 h later. We found a significant increase in extinction recall in the oxytocin group (i.e., less fear than placebo), suggesting a potential enhancement of extinction encoding/ consolidation (Acheson et al 2013). A recent study using fMRI with a very similar 1-day design of fear conditioning being followed by treatment and extinction training confirmed that within-session extinction could be enhanced by pretraining oxytocin (Eckstein et al 2014).…”

Section: Practical Considerations When Using Learned Fear Processes Asupporting

confidence: 59%

“…It has been suggested that this lack of translation of DCS effects on extinction in animals to extinction in healthy human subjects may be because extinction protocols in the laboratory are not probing "automatic" learned fear and extinction processes, but are instead governed by top-down executive functions (Grillon 2009). More recent studies, however, suggest that extinction in healthy controls is sensitive to putative extinction enhancing drugs such as cannabinoid receptor agonists and oxytocin (Acheson et al 2013;Das et al 2013;Eckstein et al 2014;Rabinak et al 2013), which suggests that these tests are "translational" in that they are sensitive to drugs that have shown efficacy in animal extinction studies (Singewald et al 2015). Whether these drugs can then also make the leap to enhancement of exposure therapy or PTSD treatment is thus far mixed.…”

Section: Pharmacological Approaches For Fear Extinction In Ptsdmentioning

confidence: 99%

“…Whether these drugs can then also make the leap to enhancement of exposure therapy or PTSD treatment is thus far mixed. Efficacy of cannabinoid receptor agonists for treating PTSD symptoms is promising (Cameron et al 2014;Roitman et al 2014), while oxytocin effects on exposure therapy are less clear (Acheson et al 2013(Acheson et al , 2015aGuastella et al 2009;Acheson and Risbrough 2015).…”

Section: Pharmacological Approaches For Fear Extinction In Ptsdmentioning

confidence: 99%

See 2 more Smart Citations

On the Road to Translation for PTSD Treatment: Theoretical and Practical Considerations of the Use of Human Models of Conditioned Fear for Drug Development

Risbrough

Glenn²,

Baker

2015

Current Topics in Behavioral Neurosciences

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The use of quantitative, laboratory-based measures of threat in humans for proof-of-concept studies and target development for novel drug discovery has grown tremendously in the last 2 decades. In particular, in the field of posttraumatic stress disorder (PTSD), human models of fear conditioning have been critical in shaping our theoretical understanding of fear processes and importantly, validating findings from animal models of the neural substrates and signaling pathways required for these complex processes. Here, we will review the use of laboratorybased measures of fear processes in humans including cued and contextual conditioning, generalization, extinction, reconsolidation, and reinstatement to develop novel drug treatments for PTSD. We will primarily focus on recent advances in using behavioral and physiological measures of fear, discussing their sensitivity as biobehavioral markers of PTSD symptoms, their response to known and novel PTSD treatments, and in the case of d-cycloserine, how well these findings have translated to outcomes in clinical trials. We will highlight some gaps in the literature and needs for future research, discuss benefits and limitations of these outcome measures in designing proof-of-concept trials, and offer practical guidelines on design and interpretation when using these fear models for drug discovery.

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Section: Practical Considerations When Using Learned Fear Processes Asupporting

confidence: 59%

Section: Pharmacological Approaches For Fear Extinction In Ptsdmentioning

confidence: 99%

Section: Pharmacological Approaches For Fear Extinction In Ptsdmentioning

confidence: 99%

See 1 more Smart Citation

On the Road to Translation for PTSD Treatment: Theoretical and Practical Considerations of the Use of Human Models of Conditioned Fear for Drug Development

Risbrough

Glenn²,

Baker

2015

Current Topics in Behavioral Neurosciences

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“…OT has anxiolytic properties both at the neurobiological and behavioral level. Behaviorally, OT administration resulted in decreased subjective anxiety during a public speaking stressor in healthy individuals (de Oliveira et al, 2012) and increased (recall of) extinction learning in both rodents (Zoicas et al, 2014) and healthy males (Acheson et al, 2013). In addition, functional MRI (fMRI) studies have shown that OT administration dampened amygdala reactivity toward emotional stimuli in healthy males (Kirsch et al, 2005), males with generalized social anxiety disorder (GSAD; Labuschagne et al, 2010) and females with borderline personality disorder (BPD; Bertsch et al, 2013), although findings for females have been mixed (Domes et al, 2010).…”

Section: Introductionmentioning

confidence: 99%

Intranasal Oxytocin Administration Dampens Amygdala Reactivity towards Emotional Faces in Male and Female PTSD Patients

Koch

Zuiden

Nawijn

et al. 2015

Neuropsychopharmacol

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Post-traumatic stress disorder (PTSD) is a disabling psychiatric disorder. As a substantial part of PTSD patients responds poorly to currently available psychotherapies, pharmacological interventions boosting treatment response are needed. Because of its anxiolytic and pro-social properties, the neuropeptide oxytocin (OT) has been proposed as promising strategy for treatment augmentation in PTSD. As a first step to investigate the therapeutic potential of OT in PTSD, we conducted a double-blind, placebo-controlled, cross-over functional MRI study examining OT administration effects (40 IU) on amygdala reactivity toward emotional faces in unmedicated male and female police officers with (n = 37, 21 males) and without (n = 40, 20 males) PTSD. Trauma-exposed controls were matched to PTSD patients based on age, sex, years of service and educational level. Under placebo, the expected valence-dependent amygdala reactivity (ie, greater activity toward fearful-angry faces compared with happy-neutral faces) was absent in PTSD patients. OT administration dampened amygdala reactivity toward all emotional faces in male and female PTSD patients, but enhanced amygdala reactivity in healthy male and female traumaexposed controls, independent of sex and stimulus valence. In PTSD patients, greater anxiety prior to scanning and amygdala reactivity during the placebo session were associated with greater reduction of amygdala reactivity after OT administration. Taken together, our results indicate presumably beneficial neurobiological effects of OT administration in male and female PTSD patients. Future studies should investigate OT administration in clinical settings to fully appreciate its therapeutic potential.

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“…fMRI studies in humans showed that a single administration of OT attenuated amygdala reactivity to negative emotional stimuli and enhanced amygdala-medial PFC resting-state FC in healthy males (Kirsch et al, 2005;Sripada et al, 2012a), and males with generalized social anxiety disorder (Dodhia et al, 2014;Labuschagne et al, 2010). Moreover, OT attenuated amygdala reactivity and increased PFC reactivity during fear extinction (Eckstein et al, 2015), and increased fear extinction recall after fear extinction training (Acheson et al, 2013) in healthy males. Similarly, OT dampened amygdala and dACC reactivity to fear-conditioned faces, while reducing negative ratings of these faces (Petrovic et al, 2008).…”

Section: Introductionmentioning

confidence: 99%

Intranasal Oxytocin Affects Amygdala Functional Connectivity after Trauma Script-Driven Imagery in Distressed Recently Trauma-Exposed Individuals

Frijling

Zuiden

Koch

et al. 2015

Neuropsychopharmacol

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Approximately 10% of trauma-exposed individuals go on to develop post-traumatic stress disorder (PTSD). Neural emotion regulation may be etiologically involved in PTSD development. Oxytocin administration early post-trauma may be a promising avenue for PTSD prevention, as intranasal oxytocin has previously been found to affect emotion regulation networks in healthy individuals and psychiatric patients. In a randomized double-blind placebo-controlled between-subjects functional magnetic resonance (fMRI) study, we assessed the effects of a single intranasal oxytocin administration (40 IU) on seed-based amygdala resting-state FC with emotion regulation areas (ventromedial prefrontal cortex (vmPFC), ventrolateral prefrontal cortex (vlPFC)), and salience processing areas (insula, dorsal anterior cingulate cortex (dACC)) in 37 individuals within 11 days post trauma. Two resting-state scans were acquired; one after neutral-and one after trauma-script-driven imagery. We found that oxytocin administration reduced amygdala-left vlPFC FC after trauma script-driven imagery, compared with neutral script-driven imagery, whereas in PL-treated participants enhanced amygdala-left vlPFC FC was observed following trauma script-driven imagery. Irrespective of script condition, oxytocin increased amygdala-insula FC and decreased amygdalavmPFC FC. These neural effects were accompanied by lower levels of sleepiness and higher flashback intensity in the oxytocin group after the trauma script. Together, our findings show that oxytocin administration may impede emotion regulation network functioning in response to trauma reminders in recently trauma-exposed individuals. Therefore, caution may be warranted in administering oxytocin to prevent PTSD in distressed, recently trauma-exposed individuals.

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The effect of intranasal oxytocin treatment on conditioned fear extinction and recall in a healthy human sample

Cited by 124 publications

References 45 publications

On the Road to Translation for PTSD Treatment: Theoretical and Practical Considerations of the Use of Human Models of Conditioned Fear for Drug Development

On the Road to Translation for PTSD Treatment: Theoretical and Practical Considerations of the Use of Human Models of Conditioned Fear for Drug Development

Intranasal Oxytocin Administration Dampens Amygdala Reactivity towards Emotional Faces in Male and Female PTSD Patients

Intranasal Oxytocin Affects Amygdala Functional Connectivity after Trauma Script-Driven Imagery in Distressed Recently Trauma-Exposed Individuals

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