The basolateral amygdala is essential for rapid escape: A human and rodent study
Publication year
2018Author(s)
Number of pages
29 p.
Source
Cell, 175, 3, (2018), pp. 723-735.e16ISSN
Publication type
Article / Letter to editor

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Organization
SW OZ BSI KLP
PI Group Affective Neuroscience
Journal title
Cell
Volume
vol. 175
Issue
iss. 3
Languages used
English (eng)
Page start
p. 723
Page end
p. 735.e16
Subject
230 Affective Neuroscience; Experimental Psychopathology and TreatmentAbstract
Rodent research delineates how the basolateral amygdala (BLA) and central amygdala (CeA) control defensive behaviors, but translation of these findings to humans is needed. Here, we compare humans with natural-selective bilateral BLA lesions to rats with a chemogenetically silenced BLA. We find, across species, an essential role for the BLA in the selection of active escape over passive freezing during exposure to imminent yet escapable threat (Timm). In response to Timm, BLA-damaged humans showed increased startle potentiation and BLA-silenced rats demonstrated increased startle potentiation, freezing, and reduced escape behavior as compared to controls. Neuroimaging in humans suggested that the BLA reduces passive defensive responses by inhibiting the brainstem via the CeA. Indeed, Timm conditioning potentiated BLA projections onto an inhibitory CeA pathway, and pharmacological activation of this pathway rescued deficient Timm responses in BLA-silenced rats. Our data reveal how the BLA, via the CeA, adaptively regulates escape behavior from imminent threat and that this mechanism is evolutionary conserved across rodents and humans.
This item appears in the following Collection(s)
- Academic publications [229196]
- Donders Centre for Cognitive Neuroimaging [3665]
- Electronic publications [111662]
- Faculty of Social Sciences [28727]
- Open Access publications [80462]
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