Your search keyword '"Hurlemann, R."' showing total 8 results

1. An Emotion-Induced Retrograde Amnesia in Humans Is Amygdala- and β-Adrenergic-Dependent

Author

Strange, B. A., Hurlemann, R., and Dolan, R. J.

Published

2003

2. Common and dissociable effects of oxytocin and lorazepam on the neurocircuitry of fear.

Author

Kreuder AK, Scheele D, Schultz J, Hennig J, Marsh N, Dellert T, Ettinger U, Philipsen A, Babasiz M, Herscheid A, Remmersmann L, Stirnberg R, Stöcker T, and Hurlemann R

Subjects

Adult, Fear physiology, Humans, Magnetic Resonance Imaging, Male, Neurotransmitter Agents pharmacology, Young Adult, Amygdala diagnostic imaging, Amygdala drug effects, Amygdala physiology, Fear drug effects, Lorazepam pharmacology, Oxytocin pharmacology

Abstract

Benzodiazepines (BZDs) represent the gold standard of anxiolytic pharmacotherapy; however, their clinical benefit is limited by side effects and addictive potential. Consequently, there is an urgent need to develop novel and safe anxiolytics. The peptide hormone oxytocin (OXT) exhibits anxiolytic-like properties in animals and humans, but whether OXT and BZDs share similar effects on the neural circuitry of fear is unclear. Therefore, the rationale of this ultra-high-field functional MRI (fMRI) study was to test OXT against the clinical comparator lorazepam (LZP) with regard to their neuromodulatory effects on local and network responses to fear-related stimuli. One hundred twenty-eight healthy male participants volunteered in this randomized double-blind, placebo-controlled, between-group study. Before scanning using an emotional face-matching paradigm, participants were randomly administered a single dose of OXT (24 IU), LZP (1 mg), or placebo. On the behavioral level, LZP, but not OXT, caused mild sedation, as evidenced by a 19% increase in reaction times. On the neural level, both OXT and LZP inhibited responses to fearful faces vs. neutral faces within the centromedial amygdala (cmA). In contrast, they had different effects on intra-amygdalar connectivity; OXT strengthened the coupling between the cmA and basolateral amygdala, whereas LZP increased the interplay between the cmA and superficial amygdala. Furthermore, OXT, but not LZP, enhanced the coupling between the cmA and the precuneus and dorsomedial prefrontal cortex. These data implicate inhibition of the cmA as a common denominator of anxiolytic action, with only OXT inducing large-scale connectivity changes of potential therapeutic relevance., Competing Interests: The authors declare no competing interest.

Published

2020

3. Oxytocin-enforced norm compliance reduces xenophobic outgroup rejection.

Author

Marsh N, Scheele D, Feinstein JS, Gerhardt H, Strang S, Maier W, and Hurlemann R

Subjects

Administration, Intranasal, Adolescent, Adult, Altruism, Female, Humans, Male, Oxytocics administration & dosage, Oxytocin administration & dosage, Prejudice, White People, Young Adult, Oxytocics pharmacology, Oxytocin pharmacology, Xenophobia psychology

Abstract

Never before have individuals had to adapt to social environments defined by such magnitudes of ethnic diversity and cultural differentiation. However, neurobiological evidence informing about strategies to reduce xenophobic sentiment and foster altruistic cooperation with outsiders is scarce. In a series of experiments settled in the context of the current refugee crisis, we tested the propensity of 183 Caucasian participants to make donations to people in need, half of whom were refugees (outgroup) and half of whom were natives (ingroup). Participants scoring low on xenophobic attitudes exhibited an altruistic preference for the outgroup, which further increased after nasal delivery of the neuropeptide oxytocin. In contrast, participants with higher levels of xenophobia generally failed to exhibit enhanced altruism toward the outgroup. This tendency was only countered by pairing oxytocin with peer-derived altruistic norms, resulting in a 74% increase in refugee-directed donations. Collectively, these findings reveal the underlying sociobiological conditions associated with outgroup-directed altruism by showing that charitable social cues co-occurring with enhanced activity of the oxytocin system reduce the effects of xenophobia by facilitating prosocial behavior toward refugees., Competing Interests: The authors declare no conflict of interest.

Published

2017

4. Oxytocin, the peptide that bonds the sexes also divides them.

Author

Gao S, Becker B, Luo L, Geng Y, Zhao W, Yin Y, Hu J, Gao Z, Gong Q, Hurlemann R, Yao D, and Kendrick KM

Subjects

Adult, Female, Humans, Magnetic Resonance Imaging, Male, Sociological Factors, Young Adult, Amygdala physiology, Oxytocin physiology, Sex Characteristics, Social Behavior

Abstract

Facilitation of social attraction and bonding by the evolutionarily conserved neuropeptide oxytocin is well-established in female mammals. However, accumulating behavioral evidence suggests that oxytocin may have evolved sex-specific functional roles in the domain of human social cognition. A critical question is how oxytocin differentially modulates neural processing of social information in men and women, leading to divergent behavioral responses. Here we show that intranasal oxytocin treatment produces sex- and valence-dependent increases in amygdala activation when women view individuals identified as praising others but in men those who criticize them. Women subsequently show increased liking for the faces of these individuals, whereas in men it is reduced. Thus, oxytocin may act differentially via the amygdala to enhance the salience of positive social attributes in women but negative ones in men. We hypothesize that oxytocin may have evolved different but complementary roles to help ensure successful reproduction by encouraging mothers to promote a prosocial rearing environment for offspring and fathers to protect against antisocial influences.

Published

2016

5. Amygdala lesions do not compromise the cortical network for false-belief reasoning.

Author

Spunt RP, Elison JT, Dufour N, Hurlemann R, Saxe R, and Adolphs R

Subjects

Adolescent, Adult, Aged, Amygdala pathology, Brain Mapping, Cognition physiology, Female, Humans, Judgment physiology, Magnetic Resonance Imaging, Male, Middle Aged, Psychomotor Performance physiology, Reaction Time physiology, Young Adult, Amygdala physiopathology, Cerebral Cortex physiology, Culture, Nerve Net physiology, Theory of Mind

Abstract

The amygdala plays an integral role in human social cognition and behavior, with clear links to emotion recognition, trust judgments, anthropomorphization, and psychiatric disorders ranging from social phobia to autism. A central feature of human social cognition is a theory-of-mind (ToM) that enables the representation other people's mental states as distinct from one's own. Numerous neuroimaging studies of the best studied use of ToM--false-belief reasoning--suggest that it relies on a specific cortical network; moreover, the amygdala is structurally and functionally connected with many components of this cortical network. It remains unknown whether the cortical implementation of any form of ToM depends on amygdala function. Here we investigated this question directly by conducting functional MRI on two patients with rare bilateral amygdala lesions while they performed a neuroimaging protocol standardized for measuring cortical activity associated with false-belief reasoning. We compared patient responses with those of two healthy comparison groups that included 480 adults. Based on both univariate and multivariate comparisons, neither patient showed any evidence of atypical cortical activity or any evidence of atypical behavioral performance; moreover, this pattern of typical cortical and behavioral response was replicated for both patients in a follow-up session. These findings argue that the amygdala is not necessary for the cortical implementation of ToM in adulthood and suggest a reevaluation of the role of the amygdala and its cortical interactions in human social cognition.

Published

2015

6. Oxytocin enhances brain reward system responses in men viewing the face of their female partner.

Author

Scheele D, Wille A, Kendrick KM, Stoffel-Wagner B, Becker B, Güntürkün O, Maier W, and Hurlemann R

Subjects

Administration, Intranasal, Face, Female, Humans, Magnetic Resonance Imaging, Male, Nucleus Accumbens drug effects, Oxytocin administration & dosage, Recognition, Psychology physiology, Ventral Tegmental Area drug effects, Interpersonal Relations, Love, Oxytocin pharmacology, Reward, Sexual Partners psychology

Abstract

The biological mechanisms underlying long-term partner bonds in humans are unclear. The evolutionarily conserved neuropeptide oxytocin (OXT) is associated with the formation of partner bonds in some species via interactions with brain dopamine reward systems. However, whether it plays a similar role in humans has as yet not been established. Here, we report the results of a discovery and a replication study, each involving a double-blind, placebo-controlled, within-subject, pharmaco-functional MRI experiment with 20 heterosexual pair-bonded male volunteers. In both experiments, intranasal OXT treatment (24 IU) made subjects perceive their female partner's face as more attractive compared with unfamiliar women but had no effect on the attractiveness of other familiar women. This enhanced positive partner bias was paralleled by an increased response to partner stimuli compared with unfamiliar women in brain reward regions including the ventral tegmental area and the nucleus accumbens (NAcc). In the left NAcc, OXT even augmented the neural response to the partner compared with a familiar woman, indicating that this finding is partner-bond specific rather than due to familiarity. Taken together, our results suggest that OXT could contribute to romantic bonds in men by enhancing their partner's attractiveness and reward value compared with other women.

Published

2013

7. Oxytocin facilitates protective responses to aversive social stimuli in males.

Author

Striepens N, Scheele D, Kendrick KM, Becker B, Schäfer L, Schwalba K, Reul J, Maier W, and Hurlemann R

Subjects

Brain physiology, Double-Blind Method, Female, Humans, Magnetic Resonance Imaging, Male, Placebos, Avoidance Learning, Oxytocin physiology

Abstract

The neuropeptide oxytocin (OXT) can enhance the impact of positive social cues but may reduce that of negative ones by inhibiting amygdala activation, although it is unclear whether the latter causes blunted emotional and mnemonic responses. In two independent double-blind placebo-controlled experiments, each involving over 70 healthy male subjects, we investigated whether OXT affects modulation of startle reactivity by aversive social stimuli as well as subsequent memory for them. Intranasal OXT potentiated acoustic startle responses to negative stimuli, without affecting behavioral valence or arousal judgments, and biased subsequent memory toward negative rather than neutral items. A functional MRI analysis of this mnemonic effect revealed that, whereas OXT inhibited amygdala responses to negative stimuli, it facilitated left insula responses for subsequently remembered items and increased functional coupling between the left amygdala, left anterior insula, and left inferior frontal gyrus. Our results therefore show that OXT can potentiate the protective and mnemonic impact of aversive social information despite reducing amygdala activity, and suggest that the insula may play a role in emotional modulation of memory.

Published

2012

8. An emotion-induced retrograde amnesia in humans is amygdala- and beta-adrenergic-dependent.

Author

Strange BA, Hurlemann R, and Dolan RJ

Subjects

Adult, Female, Humans, Language, Male, Placebos, Propranolol pharmacology, Sex Factors, Speech, Amnesia, Retrograde etiology, Amygdala metabolism, Emotions, Memory, Receptors, Adrenergic, beta metabolism

Abstract

The influence of emotion on human memory is associated with two contradictory effects in the form of either emotion-induced enhancements or decrements in memory. In a series of experiments involving single word presentation, we show that enhanced memory for emotional words is strongly coupled to decrements in memory for items preceding the emotional stimulus, an effect that is more pronounced in women. These memory effects would appear to depend on a common neurobiological substrate, in that enhancements and decrements are reversed by propranolol, a beta-adrenergic antagonist, and abolished by selective bilateral amygdala damage. Thus, our findings suggest that amygdala-dependent beta-adrenergic modulation of episodic encoding has costs as well as benefits.

Published

2003