CRF-1 receptor antagonist blockade of CRF-induced sensitization of ethanol
withdrawal-induced anxiety-like behavior from the central amygdala, dorsal
raphe, and d-BNST. A 10 mg/kg dose of the CRF-1 receptor antagonist,
SSR125543 (SSR), was administered intraperitoneally 15 min before the
microinjection of CRF (0.5 μg) into either the central amygdala
or the d-BNST followed by the 5 days of ethanol diet. Meanwhile, another
CRF-1 receptor antagonist CP154526 (CP; 10 mg/kg i.p.) was administered 15
min before each of the CRF (0.5 μg) microinjections into the
dorsal raphe. See Fig. 1 for protocol.
The action of CRF in these brain sites to induce sensitization of
withdrawal-induced anxiety-like behavior was prevented by the CRF-1 receptor
antagonist. Social interaction was measured 5 to 6 h after the ethanol diet
removal. The number of rats for each group is listed in Table 1, part 4. In the CD-vehicle group
and the ED-vehicle group, vehicle was administered into each of the brain
sites (n = 4–6 for each site), and data were
combined because a significant change across sites was not observed. No
significant difference in social interaction during ethanol withdrawal
(P > 0.05) was observed when the CD-vehicle
group was compared with the ED-vehicle group. A representation of brain
region at which CRF injections were aimed for each brain site is presented
in Supplemental Material. *, P < 0.01 compared
with vehicle CD- and vehicle ED-treated groups and the groups that received
the SSR125543 systemically [F(7,76) = 3.005,
P < 0.01].