Download Paper: Inactivation of Basolateral Amygdala Specifically Eliminates

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Transcript 
Hypothesis:
“Amygdala processing emotional information then
used by cortex to drive appropriate behavioral
responses to the stimuli”
Background:
• Gustatory cortex (GC) and basolateral amygdala (BLA) are
monosynaptically and polysynaptically connected.
• GC taste responses progress through sequences of epochs
(taste-specific spike rates with particular response latencies
and durations), which code first the presence, then the
identity, and finally the palatability of tastes.
• Response dynamics in BLA are a close match for those of GC,
in that BLA neurons switch through epochs at similar times.
Palatability-related information appearsone epoch earlier in
BLA
Materials and Methods:
• Female Long-Evans Rats served as subjects.
Theanesthetized rat was placed in a stereotaxic frame, its scalp excised, and holes
bored in its skull for the insertion of self-tapping ground screws, electrode bundles,
and guide cannulae for infusions.
• Muscimol was used to temporallly inactivate BLA.
Muscimol (100 ng/0.5 l; MP Biomedicals) or saline vehicle was infused
bilaterally into BLA at a rate of 0.25l/min for 2 min (total infusate, 0.5l).
• Neural signals were collected from GC during taste sampling.
Sample histology showing placement of electrode
tips.
Sample histology showing placement of cannula
tips centered in BLA.
Insular cortex
basolateral amygdala
The overall impact of BLAx on the
entire GC population.
BLAx changes firing rate of responses
and recover within 8 h after muscimol
infusion.
Epoch dependency of the
effects of BLAx.
Late-epoch palatability processing
is specifically affected by BLAx.
Conclusion:
Temporary inactivation of BLA (BLAx) halfway
through GC recording sessions changed taste
responses in all but a handful of GC neurons. BLAx
affected firing rates across entire responses, but
the impact was epoch-specific: Late-epoch
palatability-related information was abolished or
diminished in all but one small, identifiable subset
of neurons, while identity-related information was
left intact. Thus, BLA plays a powerful role in the
driving of palatabilityrelated responses in GC, but
the relationship between the two structures
appears to be complex.
Thanks for attention!
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