Abstract

Most sensory systems have a mechanism for comparison that, through exaggeration of perceived stimulus difference, serves to facilitate accurate detection of, and responding to, a range of stimuli. Such an effect can be demonstrated in the gustatory system by varying the temporal presentation of different concentrations of a normally preferred stimulus. Specifically, when presented in separate sessions, rats will demonstrate a concentration effect by licking more for a high than for a low concentration of sucrose. When presentation of the two concentrations is alternated within the same session, however, the concentration effect is exaggerated 2-3 times. In behavioral studies this exaggeration in referred to as a Simultaneous Contrast Effect. That is, licking for the high concentration is enhanced (positive contrast) and licking for the low concentration is suppressed (negative contrast) when rats are given the opportunity to compare the two closely in time. This effect can be likened to an""""""""edge effect"""""""" in the visual system. Despite the likely contribution of such comparison effects to detecting, coding, and responding to gustatory stimuli, the behavioral and electrophysiological assessment of taste processing has been limited to investigation during conditions designed to prevent stimulus comparison. For example, behavioral responsiveness to stimulus quality and intensity typically is evaluated using random stimulus delivery in an effort to reduce the potential effects of prior experience on ingestive behavior. During electrophysiological experiments, a similar attempt is made to eliminate order effects by presenting the stimuli in a rinse-stimulus-rinse sequence. The present proposal seeks to establish the neural basis for this comparison process. Preliminary data indicate that an intact brainstem is sufficient to mediate the behavioral expression of Simultaneous Contrast Effects. Other experiments, however, discount adaptation of the peripheral receptors as an explanation of the phenomenon and rule out involvement of the pontine parabrachial nuclei. This leaves the nucleus of the solitary tract (NST) as a potential site for the neural mechanisms that produce athe effect. In fact, our preliminary data demonstrate exaggerated responses to alternating concentrations of sucrose, NaCl, or citric acid in NST units. This effect occurs for sucrose even when the two concentrations are applied to separate receptive fields, further discounting an adaptation interpretation of the phenomenon. The focus of this proposal is to: (1) select the sucrose concentration pair associated with the largest contrast effects in behavior; (2) examine the effect of comparison and non-comparison conditions (using the Simultaneous Contrast procedure) on gustatory coding in NST units; (3) determine the parametric constraints on contrast effects both behaviorally and electrophysiologically; and (4), extend pilot data that rule out peripheral adaptation as the sole mechanism for Simultaneous Contrast.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute on Deafness and Other Communication Disorders (NIDCD)
Type
First Independent Research Support & Transition (FIRST) Awards (R29)
Project #
5R29DC002016-03
Application #
2654413
Study Section
Sensory Disorders and Language Study Section (CMS)
Project Start
1996-02-01
Project End
2001-01-31
Budget Start
1998-02-01
Budget End
1999-01-31
Support Year
3
Fiscal Year
1998
Total Cost
Indirect Cost

  Institution

Name
Pennsylvania State University
Department
Neurosciences
Type
Schools of Medicine
DUNS #
129348186
City
Hershey
State
PA
Country
United States
Zip Code
17033

  Publications

Grigson, Patricia Sue; Twining, Robert C (2002) Cocaine-induced suppression of saccharin intake: a model of drug-induced devaluation of natural rewards. Behav Neurosci 116:321-33
Grigson, P S; Wheeler, R A; Wheeler, D S et al. (2001) Chronic morphine treatment exaggerates the suppressive effects of sucrose and cocaine, but not lithium chloride, on saccharin intake in Sprague-Dawley rats. Behav Neurosci 115:403-16
Sclafani, A; Azzara, A V; Touzani, K et al. (2001) Parabrachial nucleus lesions block taste and attenuate flavor preference and aversion conditioning in rats. Behav Neurosci 115:920-33
Gomez, F; Leo, N A; Grigson, P S (2000) Morphine-induced suppression of saccharin intake is correlated with elevated corticosterone levels. Brain Res 863:52-8
Grigson, P S; Freet, C S (2000) The suppressive effects of sucrose and cocaine, but not lithium chloride, are greater in Lewis than in Fischer rats: evidence for the reward comparison hypothesis. Behav Neurosci 114:353-63
Grigson, P S; Lyuboslavsky, P; Tanase, D (2000) Bilateral lesions of the gustatory thalamus disrupt morphine- but not LiCl-induced intake suppression in rats: evidence against the conditioned taste aversion hypothesis. Brain Res 858:327-37
Grigson, P S; Twining, R C; Carelli, R M (2000) Heroin-induced suppression of saccharin intake in water-deprived and water-replete rats. Pharmacol Biochem Behav 66:603-8
Grigson, P S; Lyuboslavsky, P N; Tanase, D et al. (1999) Water-deprivation prevents morphine-, but not LiCl-induced, suppression of sucrose intake. Physiol Behav 67:277-86
Gomez, F; Grigson, P S (1999) The suppressive effects of LiCl, sucrose, and drugs of abuse are modulated by sucrose concentration in food-deprived rats. Physiol Behav 67:351-7
Grigson, P S; Reilly, S; Scalera, G et al. (1998) The parabrachial nucleus is essential for acquisition of a conditioned odor aversion in rats. Behav Neurosci 112:1104-13

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