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The Journal of Neuroscience, October 1, 2002, 22(19):8748-8753
Amygdalo-Hypothalamic Circuit Allows Learned Cues to Override Satiety and Promote Eating
Gorica D. Petrovich, Barry Setlow, Peter C. Holland, and Michela Gallagher Department of Psychological and Brain Sciences, Johns Hopkins University, Baltimore, Maryland 21218
ABSTRACT
TOP
ABSTRACT
INTRODUCTION
Organisms eat not only in a response to signals related to energy balance. Eating also occurs in response to "extrinsic," or environmental, signals, including learned cues. Such cues can modify feeding based on motivational value acquired through association with either rewarding or aversive events. We provide evidence that a specific brain system, involving connections between basolateral amygdala and the lateral hypothalamus, is crucial for allowing learned cues (signals that were paired with food delivery when the animal was hungry) to override satiety and promote eating in sated rats. In an assessment of second-order conditioning, we also found that disconnection of this circuitry had no effect on the ability of a conditioned cue to support new learning. Knowledge about neural systems through which food-associated cues specifically control feeding behavior provides a defined model for the study of learning that may be informative for understanding mechanisms that contribute to eating disorders and more moderate forms of overeating.
Key words: amygdala; hypothalamus; eating; feeding behavior; learning; goal-directed behavior; motivation
INTRODUCTION
Mild to severe obesity, estimated to affect ~60% of the adult population in developed countries, is a risk factor for a range of diseases (United States Department of Health and Human Services, 1999). Despite adverse health consequences, difficulties in achieving and maintaining weight control are common. Overeating is attributable, at least in part, to the fact that food consumption is powerfully influenced by a variety of environmental factors that are unrelated to energy requirements (Rodin, 1981
; Booth, 1989
Recent research is beginning to define the neural systems through which such psychological processes influence eating. Under conditions that strongly potentiate feeding, laboratory rats with neurotoxic lesions of the basolateral amygdalar area (BLA) [including basolateral ("basal"), basomedial ("accessory basal"), and lateral nuclei] fail to increase eating in the presence of a conditioned stimulus (CS) that was previously paired with food (Gallagher, 2000
The current investigation examined potentiation of feeding by a CS in rats with a preparation that disconnects the BLA and the LHA. Here we report that the BLA-LHA system is crucial for allowing learned cues to override satiety signals and stimulate eating in sated states. We further show that the BLA-LHA system is specifically important for the control of eating by learned signals, because it does not regulate baseline eating or the rate at which rats gain weight when fed ad libitum.
MATERIALS AND METHODS
Subjects. Experimentally naive, male Long-Evans rats (Charles River Laboratories, Raleigh, NC), weighing ~300 gm on arrival in the vivarium, were individually caged, maintained on a 12 hr light/dark cycle, and given ad libitum access to food and water, except as otherwise noted. After 1 week acclimation to vivarium conditions, during which time they were handled extensively, rats were given contralateral, ipsilateral, or sham-contralateral lesions of BLA and LHA and then allowed to recover for 1 week before undergoing behavioral procedures.
Surgical methods. All surgeries were performed under aseptic conditions using isoflurane gas for induction and maintenance of anesthesia, using a stereotaxic frame (Kopf Instruments, Tujunga, CA). Neurotoxic unilateral lesions were made with NMDA (Sigma, St. Louis, MO) in a 0.1 M phosphate buffer solution, using a concentration of 12.5 mg/ml for BLA and 20 mg/ml for LHA lesions. The placement of lesions was balanced, such that there were approximately equal numbers of rats with lesions in the left or right hemispheres in each group. For BLA, a total of 0.3 µl was infused [the flat skull coordinates from bregma were as follows: anteroposterior (AP),
2.70 mm; mediolateral (ML), ±4.80 mm; and dorsoventral (DV),
Apparatus. Six identical behavioral chambers (30 × 24 × 30 cm; Colbourn Instruments, Allentown, PA), each with a grid floor, aluminum top and sides, and a transparent Plexiglas back and front, were used for training and testing. The interior length of each chamber was reduced by positioning a transparent Plexiglas partition at an angle such that the length of the floor was reduced to 22 cm, but the length at the top of the box remained unaltered. On the side wall opposite the Plexiglas partition, each chamber contained a recessed food cup (3.2 × 4.2 cm), into which food pellets (45 mg; P. J. Noyes, Lancaster, NH) were delivered. Dim background illumination was provided by two 25 W red bulbs, each placed ~1.5 m from the test chambers. Masking noise (60 dB) was provided by ventilation fans located outside each box. A 10 sec tone (1500 Hz, 70 dB) and a 10 sec white noise (70 dB) were used as CS+ and CS
Video cameras attached to videocassette recorders were placed 1 m in front of the test chambers to record behavior for a 10 sec period before and during stimulus presentation. Stimulus presentation and videocassette recorders were controlled by LabView (National Instruments) software run on Macintosh computers (Apple Computers, Cupertino, CA).
Behavioral procedures. Before behavior training, rats were gradually reduced to 85% of their ad libitum weights. After a shaping procedure (Setlow et al., 2002
After completion of first-order conditioning, rats were given 9 d of ad libitum access to food in their home cage. On the last two of these days, the rats received consumption tests (one per day) in the test chambers: one with the CS+ and the other with CS
After the completion of tests for CS potentiation of feeding, all rats were again gradually reduced to 85% of their current ad libitum weights and then received two "reminder" sessions of CS+-food pairings (identical to the first two training sessions; see above). For second-order conditioning, each of the original groups (sham, ipsilateral, and contralateral) was subdivided into a "paired" group, which received presentations of the 10 sec light CS2 paired with (immediately followed by) the first-order CS+, and an "unpaired" group, which received the same number of light and CS+ presentations that were explicitly unpaired. The unpaired groups were included to control for non-associative increases in responding to the light CS2. For both paired and unpaired groups, the first half of session 1 began with a CS+-food reminder trial, followed by three presentations of the light alone to evaluate unconditioned responding to the light. In the second half of session 1, as well as in each half of sessions 2-8, the paired groups received three trials of the light CS2 paired with the auditory CS+; the unpaired groups received three trials each of auditory CS+ and light CS2 unpaired. All groups also received one CS+-food reminder trials in each half session.
Behavioral observations. Observations were made from the videotapes of the behavioral conditioning sessions by experimenters who were "blind" to group assignments. The observations were paced by auditory signals (at 1.25 sec intervals) recorded onto the tapes. At each observation, only one behavior was recorded. The primary measure of conditioning [conditioned responses (CRs)] to the auditory (in the first-order discrimination phase) and visual (in the second-order conditioning phase) CSs, was the percentage of time the rats spent expressing food cup behavior during the CS intervals. Food cup behavior consists of nose pokes into the recessed food cup, standing motionless in front of the food cup, or short, rapid, horizontal, or vertical head jerks (in the vicinity of the food cup).
Statistics. Behavioral data were analyzed using nonparametric statistics (Kruskall-Wallis, Mann-Whitney, and Wilcoxon signed-rank tests when appropriate). In all cases, p < 0.05 was considered significant.
Histological procedure. After completion of all behavioral procedures, rats were given an overdose of pentobarbital (100 mg/kg) and perfused intracardially with 0.9% saline, followed by 4% Formalin in 0.1 M PBS. The brains were removed and stored in the Formalin solution used for perfusion for 48-72 hr and then transferred to 12% sucrose in 0.1 M PBS for 24 hr. The brains were sliced on a freezing microtome, and coronal sections (40 µm) collected through the areas of the BLA and LHA were mounted on slides and Nissl stained. Lesion placements were verified under a light microscope and drawn onto plates adapted from the atlas of Swanson (1992)
RESULTS
Histology
The BLA-LHA system was disconnected by making asymmetrical lesions (unilateral lesions of BLA and LHA on opposite sides of the brain), using the neurotoxin NMDA (Fig. 1A,B). Because BLA outputs are predominantly ipsilateral (McDonald and Culberson, 1986
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Figure 1. Histology. A, The extent of the largest (enclosed black area) and smallest (filled black area) acceptable lesions at several rostrocaudal levels for all rats in the contralateral and ipsilateral groups. Except for minor mechanical damage along the injector tracks, no damage was evident in any of the sham-lesioned brains. Plates adapted from the atlas of Swanson (1992)
Lesions were rejected if there was <50% damage to BLA or LHA or if there was more than minimal (>10%) damage to the adjoining regions (the central nucleus and cortical regions for the BLA, and medial hypothalamus and thalamus for the LHA). In most cases, the BLA lesions were confined specifically to the basolateral nucleus (also referred to as basal nucleus), with some additional damage to the lateral and basomedial (accessory basal) nuclei in the case of the largest lesions (Fig. 1A). The median extent of damage for acceptable lesions was ~70% in the BLA and ~75% in the LHA. Within the BLA, in all acceptable lesions, there was >90% damage to the basolateral nucleus specifically. There were no differences in size or location between the ipsilateral and contralateral lesions of the BLA or LHA.
Behavior: CS potentiation
The disconnection of the BLA-LHA system did not affect auditory Pavlovian discrimination learning (first-order conditioning). All groups of rats acquired discrimination rapidly as shown in Figure 2. CRs directed to the food cup during the occurrence of an auditory CS that predicted food delivery (CS+) were significantly elevated compared with CRs during another auditory stimulus that was not paired with food (CS
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Figure 2. First-order conditioning. Acquisition of discrimination between the CS+ and CS ), ipsilateral (
), or sham (
) lesions of the BLA and LHA. Conditioned responses to the CS+ are represented by filled symbols, and conditioned responses to the CS
After Pavlovian auditory discrimination training, which was conducted in a food-restricted state, rats were allowed food ad libitum for 1 week. Consumption tests for potentiated feeding were then performed in the sated condition on 2 consecutive days, when food was available in the test apparatus in the presence of either the CS+ or the CS
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Figure 3. Food consumption tests. A, Food consumption of sham, ipsilateral, and contralateral rats during the potentiated eating tests. Black bars show food consumption during the tests with CS+, and white bars show consumption during the tests with CS
It is also important to note that we did not find any difference in food consumption among the groups (H(2) = 0.460; p = 0.7946) during a pretesting interval in the absence of either the CS+ or the CS
Behavior: second-order conditioning
Our results demonstrate that BLA and LHA are critical components of a system through which learned cues override satiety and increase eating. It is not certain, however, that direct projections from BLA to LHA are used for this function. Indeed, BLA has a major projection to the nucleus accumbens (ACB), which in turn innervates LHA (Kirouac and Ganguly, 1995
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Figure 4. Second-order conditioning. Acquisition of second-order conditioned responses (food cup behavior) to the light CS2 during the second phase of training in rats with contralateral (
DISCUSSION
The present study demonstrated that the BLA-LHA system is crucial for allowing learned cues to override satiety signals and stimulate eating in sated states. This was attributable to an associative process in that eating was augmented by a cue paired previously with food (CS+) but not an unpaired cue (CS
If direct projections from the amygdala complex to the hypothalamus mediate the effects of learning on food consumption, that output is likely to arise from the BLA. Although other forms of associative learning, such as fear conditioning, are mediated via projections from the amygdala central nucleus, which receives a large input from the BLA (LeDoux, 2000
A substantial output from the BLA, which originates primarily in the basolateral nucleus, directly innervates the LHA (Petrovich et al., 2001
The exact LHA neurons innervated by the BLA inputs are not known at this time. Nevertheless, it is tempting to speculate that BLA outputs could influence LHA subsystems important for initiation of feeding. For example, groups of LHA neurons express two recently discovered neuropeptides, melanin concentrating hormone and orexin, which are regulated by hunger-satiety state and are linked to initiation of feeding (for review, see Elmquist et al., 1999
In addition to the projections to the LHA, the BLA outputs could reach other parts of the feeding circuit as demonstrated recently with viral labeling techniques (DeFalco et al., 2001
At the same time, it should be noted that our results do not provide a precise map of how information from the BLA reaches the LHA to modulate feeding in the potentiation paradigm. In addition to direct innervation of the LHA, as mentioned above, the BLA has a major projection to the ACB, which plays a role in feeding behavior at least in part via its connections with the LHA (Kelley, 1999
In the context of the current findings and a large body of previous work (Davis, 1992
The present results provide evidence that the amygdalo-hypothalamic system mediates learned motivational control of feeding. Experience and learning can serve an adaptive function in ingestive behavior, ranging from modifications in an organism's ingestion of particular food items, such as acquired taste aversions or taste preferences, to adaptations in how organisms use information to guide complex behavioral repertoires, such as foraging strategies. In the conditioned potentiation paradigm, cues associated with hunger acquire motivational properties to promote eating even in sated states. Given that food scarcity can occur in natural settings, cues associated with hunger in the past could serve an adaptive function by increasing the tendency to eat.
In addition to BLA inputs that access feeding circuitry in the hypothalamus, the BLA also provides innervation of topographically distinct regions of the hypothalamus implicated in the regulation of other species-typical functions, such as reproductive and defensive behaviors (Petrovich et al., 2001
The function of the BLA in the regulation of eating may also have maladaptive consequences. Learned cues that promote eating in food-sated subjects are of special relevance to natural conditions that may induce overeating. Studies in both laboratory animals and humans show that external cues associated previously with food (learned cues) exert powerful control over feeding behavior. Learned cues can override regulatory signals linked to energy balance (Weingarten, 1983
FOOTNOTES Received May 20, 2002; revised July 8, 2002; accepted July 15, 2002.
This work was supported by grants from the National Institutes of Health. We thank Summer Nugent for excellent technical support and Dr. Jennifer Bizon for comments on a previous version of this manuscript.
Correspondence should be addressed to Michela Gallagher, Department of Psychological and Brain Sciences, Johns Hopkins University, 3400 North Charles Street, Baltimore, MD 21218. E-mail: michela{at}jhu.edu.
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Copyright © 2002 Society for Neuroscience 0270-6474/02/22198748-06$05.00/0
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