SEROTONERGIC CHARACTERIZATION OF ETHANOL WITHDRAWAL
Project Number5R01AA010545-03
Contact PI/Project LeaderLAL, HARBANS
Awardee OrganizationUNIVERSITY OF NORTH TEXAS HLTH SCI CTR
Description
Abstract Text
This proposal seeks to expand experiments on characterizing ethanol
withdrawal with respect to its symptoms and their mechanisms. Abuse of
ethanol produces dependence characterized by a pattern of withdrawal
consisting of subjective symptoms such as anxiety. Although the key role
of these symptoms in initiating and maintaining ethanol abuse is well
recognized, animal research on the subjective symptoms has been
difficult. In the current funding period, it was demonstrated that
ethanol withdrawal produces a PTZ-like internal stimulus that can be used
to produce parametric data on the subjective symptoms of withdrawal. The
HZ-like stimulus occurring during ethanol withdrawal was modulated by
drugs acting at the gamma-amino butyric acid-type A (GABAA) receptor-
chloride ion channel complex. However, PTZ-IDS was insensitive to
modulation of brain serotonin (5HT) systems. The 5HT systems have been
implicated in ethanol dependence and found important in our own
experiments employing other behavioral measures. In order to better
characterize the role of 5HT in the development of ethanol dependence and
withdrawal using drug discrimination approach, new experiments are
proposed to employ a 5HT agonist, 1(3-chlorophenyl)piperazine, mCPP, as
a discriminative stimulus to characterize an animal model of the
withdrawal symptoms. It is proposed: 1) to demonstrate that the mCPP IDS
in animals is modulated by drugs which are either anxiogenic or
anxiolytic in humans, 2) to demonstrate and characterize the spontaneous
occurrence of a mCPP-like stimulus during ethanol withdrawal in relation
to the intensity of the stimulus as a function of cumulative ethanol
dose, 3) to modify the withdrawal stimulus by selected 5HT receptor
subtype agonists and antagonists, and 4) to compare and contrast the PTZ
and mCPP stimuli during ethanol withdrawal to determine the manner in
which the 5HT and GABA systems relate to one another in producing
"anxiety"-like behavior. Use of this method will provide important new
data and extend the results obtained in our other animal models of
anxiety. This research is significant because it provides information
directly related to etiology and treatment of ethanol abuse.
National Institute on Alcohol Abuse and Alcoholism
CFDA Code
273
DUNS Number
110091808
UEI
JE8AKPCR2KA4
Project Start Date
01-June-1995
Project End Date
31-May-2000
Budget Start Date
01-June-1997
Budget End Date
31-May-2000
Project Funding Information for 1997
Total Funding
$147,380
Direct Costs
$107,876
Indirect Costs
$39,504
Year
Funding IC
FY Total Cost by IC
1997
National Institute on Alcohol Abuse and Alcoholism
$147,380
Year
Funding IC
FY Total Cost by IC
Sub Projects
No Sub Projects information available for 5R01AA010545-03
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