Lesions of the dorsal hippocampal formation interfere with background but not foreground contextual fear conditioning.
Author(s) -
Russell G. Phillips,
Joseph E. LeDoux
Publication year - 1994
Publication title -
learning and memory
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 1.228
H-Index - 136
eISSN - 1549-5485
pISSN - 1072-0502
DOI - 10.1101/lm.1.1.34
Subject(s) - conditioning , psychology , classical conditioning , fear conditioning , neuroscience , hippocampal formation , stimulus (psychology) , neutral stimulus , unconditioned stimulus , measures of conditioned emotional response , dorsum , contextual learning , reinforcement , associative learning , cognitive psychology , stimulus control , social psychology , amygdala , medicine , anatomy , pedagogy , statistics , mathematics , nicotine
The effects of hippocampal lesions on the conditioning of fear responses (freezing responses) to contextual stimuli (static, continuously present stimuli) were examined in three conditioning paradigms: forward pairing of a phasic tone conditioned stimulus (CS) with a footshock unconditioned stimulus (US), unpaired presentations of the CS and US, or presentations of the US alone. All three procedures resulted in the acquisition of conditioned freezing to contextual stimuli. Lesions of the dorsal hippocampus prevented the acquisition of contextual conditioning in the Paired procedure, as reported previously, but not in the Unpaired or US Alone procedures. In the Paired procedure, static contextual cues occur in the background, with the phasic tone CS being the primary stimulus that enters into the association with the US. However, in the other two procedures, where there is no phasic CS, the primary associations with the US involve static contextual stimuli, which are therefore in the foreground. We refer to these types of contextual conditioning as background and foreground contextual conditioning, respectively, and argue that the hippocampus is only involved in background contextual conditioning. These results have implications for understanding both fear conditioning and hippocampal function.
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