Emotional memory Flashcards
Little Albert study
After 7 exposures to white rat (which previously elicited zero fear response) paired with hitting a metal bar (which caused checked breathing, arms raised, startle), presentation of rat alone caused Albert to cry and crawl away.
5 days later, they presented him with play blocks - no fear. Rats and rabbit - full fear response
Santa claus mask, dog, fur coat, cotton wool - milder fear response
He was then removed from hospital, so they couldn’t test attempts to remove the fear.
Pavlovian conventional nomenclature
Neutral stimulus can cause orientation but not the unconditioned response (salivation).
After conditioning, the neutral stimulus becomes the conditioned stimulus.
Once the conditioned stimulus elicits the full UR, it is said to have replaced the US. This is ‘stimulus substitution’.
The CS-US stimulus substitution confers info about the sensory qualities of the US, ‘US value’.
The CS-UR association, on the other hand, is a simple stimulus-response and confers no info about the US identity.
CS-UR - CeN mediated, resistant to reinforcer (US) devaluation, cannot support second order conditioning or instrumental responding.
CS-US - BLA mediated, sensitive to reinforcer devaluation, supports second order conditioning and instrumental responding.
Translationality
The ‘central fear state’ elicited in animals shares many of the same physiological symptoms to the human fear response - SCR, increased heart and ventilation rate, cessation of movement.
Experimental methods
LeDoux’s cued fear conditioning (measures fear. Problems - the freezing response is not quite the UR, bc rats don’t freeze to footshock)
Davis’s potentiated startle (measures anxiety)
The search for the neurobiological basis of fear
LeDoux 1985 - lesioning auditory cortex of rat had no effect on auditory fear conditioning. Lesioning thalamus and midbrain (both upstream) did. So where does auditory thalamus project to other than auditory cortex? LeDoux used tracing to identify subcortical sites, lesioned them in turn. The only one that affected conditioning was the amygdala.
CeN amygdala projections and their functions
lateral hypothalamus—>sympathetic activation
Dorsal motor nucleus of vagus —> parasym activation (ulcers, urination)
VTA —> DA mediated behavioural arousal
PAG —> freezing
nucleus reticularis pontis caudalis—>augmented startle response
Kapp 1979 - lesioning CeN disrupted heart rate increases in auditory fear conditioning in rabbits.
BLA functions
LeDoux lesions - impaired fear conditioning
Davis lesions - impaired potentiated startle response
So BLA responsible for sensory integration and computation.
Redundant auditory fear pathways - what are they?
From medial geniculate nucleus of thalamus to
a) auditory cortex, then auditory association cortex, then lateral nucleus amygdala
b) straight to lateral nucleus amygdala
Same thing occurs for visual conditioning - superior colliculus, to pulvinar nucleus, to BLA.
Redundant auditory fear pathways - how were they discovered?
Romanowski and LeDoux 1992 - lesioning just cortex spares conditioning to a single tone. Severing just connections from thalamus to amygdala spares conditioning to a single tone. So two separate pathways.
Jarrell et al 1987 - conditioned to two tones, one paired with footshock, the other not. Lesioning the cortex made animals freeze to both tones - so the discrimination was gone, but the tone-fear association was still there.
Redundant auditory fear pathways - why are they useful?
- optimising transmission speeds
- safety - if one fails, we’ll still respond to threats
- thalamo-cortico-amygdala pathway required for discrimination, thalamo-amygdala pathway for quick response
- representational accuracy - thalamo-amygdala connections come from associated, unaligned nuclei in the thalamus such as PIN [posterior intralaminar nucleus]. Projections to the cortex come from these associated unaligned nuclei AND from main sensory nuclei i.e. ventral medial geniculate. So the thalamo-amygdala system has a limited processing capacity in comparison.
[the main sensory vs associated sensory unaligned dissociation was proposed by Winter and Morest 1983, and supported by Romanowski and LeDoux]
Hippocampus and contextual conditioning
Lesions of hippocampus impair freezing to context, but not to CS. Amygdala lesions impair both.
COntroversy though:
- is the hippocampus just required for performance of the UR? It does induce hyperactivity…
-some lesions produce retrograde but not anterograde amnesia (i.e. pretraining lesions don’t impair conditioning)
-lesioning the entire hippocampus can impair freezing to context /and/ CS.
-McNish et al 1997 - lesioning hippocampus does not impair fear-potentiated startle
-McNish et al - lesioning hippocampus does not disrupt contextual blocking
Blanchard et al 1977 - Hippocampal lesions impaired unconditioned freezing (in response to a cat)
Intercalated cell mass
GABA-ergic cells between lateral and central nucleus. Medial ICM cells tonically inhibit CeN. LA causes lateral ICM cells to release GABA, onto the medial portion of ICM. This inhibits their inhibition, disinhibiting the CeN.
Extinction - neurological basis
VMPFC lesions impair extinction of cue-conditioning, but not contextual conditioning. [In fact, they impair recall of extinction - rats extinguish as normal, but the CS-no-US association is forgotten]
In humans, VMPFC thickness and activity is correlated with fear extinction
In rats, infralimbic bursting predicts recall of extinction two days later
Klavir et al 2012 - LFS inactivated dACC in rhesus monkeys, found better recall of extinction.
PFC projects onto extinction neurons in amygdala, which inhibit CeN from driving into fear state.
hippocampus inhibits these extinction neurons, so disinhibits CeN neurons.
PFC promotes extinction, hippocampus prevents it.
Amygdala and fear in humans
Bechara et al 1995 - patients with amygdala damage learn a CS-US pairing but do not fear condition to it. Note that these patients were quite heterogenous though.
Delgado et al 2006 - fMRI studies have found amygdala activity in instructed fear conditioning (i.e. no actual shocks delivered, just told that a stimulus would predict a shock)
Serial model of amygdala organisation - what is it?
Inputs to BLA, BLA processes and performs relevant computations (CS-US), BLA modulates CeN activity to generate output, CeN generates central fear state
