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Research statement-
We are studying the neurotransmitter serotonin. In particular, we
are interested in its role in depression and the possibility that
persistent changes in the regulation of serotonin release are involved
in adaptation to prolonged stress. Using in vivo microdialysis for
measurement of extracellular serotonin in the brain, we have studied
the influence of synaptic inputs and antidepressant drugs on serotonin
release. Drugs like Prozac that block serotonin reuptake are effective
in treating depression, but recovery is often slow. Our results
indicate that reuptake inhibitors produce an immediate small increase
in extracellular serotonin which is enhanced after prolonged administration.
We have suggested that antidepressant drug treatment alters the
strength of synaptic connections that regulate serotonin neurons.
Because little is known, we have investigated the role of the neurotransmitters
that may be involved in regulating serotonin release.
We were particularly
interested in studying glutamate because this neurotransmitter is
involved in synaptic plasticity in other brain sites. We found that
glutamate can strongly stimulate serotonin release through activation
of NMDA and AMPA receptors. However, our results indicate that these
receptors do not have a strong tonic influence on serotonin. In
contrast, the neurotransmitter GABA strongly inhibits serotonin
release in vivo. Furthermore, our results indicate that opioids
inhibit GABA release. Thus, endogenous opioids and opiate drugs
such as morphine may indirectly stimulate serotonin release as a
result of inhibiting GABA. However, after prolonged exposure, serotonin
neurons become tolerant to the stimulatory effect of morphine, and
serotonin release is inhibited during opiate withdrawal. We are
currently investigating the cellular mechanisms that could be involved
in this change and thus play a role in adaptation to prolonged stress
as well as addiction to opiate drugs.
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For complete list: PubMed
Tao, R., Ma., Z. and Auerbach, S.B. (2000)
Differential effect of local infusion of serotonin reuptake inhibitors
in the raphe versus forebrain and the role of depolarization-induced
release in increased serotonin.
J. Pharmacol. Exp. Ther. 294: 571-579.
Hjorth, S., Bengtsson, H.J., Kullberg, A., Carlzon, D., Peilot,
H. and Auerbach, S.B. (2000)
Serotonin autoreceptor function and antidepressant drug action.
J. Psychopharmacol. 14: 177-185.
Tao, R. and Auerbach, S.B. (2002)
Opioid receptor subtypes differentially modulate serotonergic neurons
in the rat CNS.
J. Pharmacol. Exp. Ther. 303: 549-556.
Tao, R. and Auerbach, S.B. (2002)
GABAergic and glutamatergic afferents in the dorsal raphe nucleus
mediate morphine-induced increases in serotonin efflux in the rat
CNS.
J. Pharmacol. Exp. Ther. 303: 704-710.
Tao, R. and Auerbach, S.B. (2003)
Influence of inhibitory and excitatory inputs on serotonergic neurons
differs in the dorsal and medial raphe nuclei.
Brain Res. 961: 109-120.
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