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157


LOW-FREQUENCY STIMULATION OF THE SUPERIOR COLLICULUS ALTERS RESPONSES SELECTED FOR INITIATION BUT DOES NOT TRIGGER SACCADES [Meeting Abstract]

GLIMCHER, PW; SPARKS, DL
ISI:A1992HK13503311
ISSN: 0146-0404
CID: 2754772

Movement selection in advance of action in the superior colliculus

Glimcher, P W; Sparks, D L
The primate superior colliculus contains a map of saccadic eye movements. Saccades are high-velocity eye movements to selected targets in the visual field, but little is known about the neural mechanisms responsible for target selection or the related problem of choosing a particular movement from the oculomotor repertoire. Two classes of neurons have been described in the superior colliculus which show bursts of activity before the saccade: discrete bursters display a vigorous pre-saccadic burst and prelude bursters show low-frequency activity as a prelude to burst onset. We have designed experiments to test whether prelude activity is related to saccade selection. Our tasks use a cue to specify which of two physically identical visual stimuli is the goal of an impending saccade. This cue is spatially and temporally isolated from the potential targets as well as from visual cues signalling movement initiation. Our results show that prelude activity occurs shortly after information is available for correct saccade selection and, more importantly, the activity is predictive of saccade choice. The results thus suggest that the superior colliculus participates in the process of saccade selection.
PMID: 1741032
ISSN: 0028-0836
CID: 199372

COLLICULAR REPRESENTATION OF MULTIPLE TARGETS - ACTIVITY OF SACCADE RELATED BURSTERS DURING AVERAGING SACCADES [Meeting Abstract]

GLIMCHER, PW; SPARKS, DL
ISI:A1991FC76201128
ISSN: 0146-0404
CID: 2754762

Neurotensin self-injection in the ventral tegmental area

Glimcher, P W; Giovino, A A; Hoebel, B G
Earlier work with the conditioned place-preference paradigm suggested that neurotensin (NT) acts as a behavioral reinforcer when microinjected into the ventral tegmental area (VTA) of the midbrain. We report here that animals will perform an operant task to obtain microinfusions of NT into the VTA. Rats reliably pressed a lever to obtain NT infusions while neglecting an identical but inactive lever. Substitution of saline for NT initiated response extinction; following the reintroduction of NT, reliable responding resumed. These results extend earlier work suggesting that NT in the VTA can be a positive reinforcer.
PMID: 3828807
ISSN: 0006-8993
CID: 199382

Endogenous opiate reward induced by an enkephalinase inhibitor, thiorphan, injected into the ventral midbrain

Glimcher, P W; Giovino, A A; Margolin, D H; Hoebel, B G
Opiates are known to be reinforcing when injected into the ventral tegmental area (VTA). The present study produced conditioned reinforcement with local injections of exogenous d-ala2-met5-enkephalinamide (DALA), a potent analogue of met-enkephalin, and with thiorphan , an enkephalinase inhibitor which protects endogenous opiates from enzymic degradation. In a conditioned place preference paradigm, rats received injections of DALA (1.0, 3.0, or 8.0 micrograms), thiorphan (60 micrograms), and/or naloxone (10 micrograms), or saline vehicle. Conditioned reinforcement was obtained with 8.0 micrograms of DALA and also with thiorphan but not with thiorphan plus naloxone. This suggests that reward can be generated by endogenous opiates in the VTA. Tests during the light phase and dark phase suggested that diurnal periodicity may play a role in opiate reward. It is concluded that the VTA can generate conditioned reward through transmitter-receptor interaction involving an endogenous opiate substrate which is probably enkephalinergic.
PMID: 6586195
ISSN: 0735-7044
CID: 199392

Neurotensin: a new 'reward peptide'

Glimcher, P W; Margolin, D H; Giovino, A A; Hoebel, B G
oeurotensin (NT) is a tridecapeptide which is thought to bind to receptors located on dopamine cells in the ventral tegmental area (VTA). Rats with cannulas implanted in the VTA showed a significant increase in time spent in an environment in which they had received bilateral injections of neurotensin on previous days. This is indicative of conditioned reinforcement in which the neuropeptide was the primary reinforcer. In order to determine the specificity of neurotensin receptor interactions, 3 fragments of the peptide were examined at 2 doses. NT1-8 and NT8-13 were found to be inactive while NT1-11 demonstrated significant activity. The results suggest that NT in the VTA is capable of inducing reinforcing effects. This is the first evidence for a non-opiate 'reward peptide'.
PMID: 6320951
ISSN: 0006-8993
CID: 199402

REWARDING EFFECTS OF NEUROTENSIN IN THE BRAIN

GLIMCHER, P; MARGOLIN, D; HOEBEL, BG
ISI:A1982QD55600046
ISSN: 0077-8923
CID: 2754732