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The Journal of Neuroscience, January 1, 2003, 23(1):23-28
BRIEF COMMUNICATION
Temporary Inactivation of the Bed Nucleus of the Stria Terminalis But Not of the Amygdala Blocks Freezing Induced by Trimethylthiazoline, a Component of Fox FecesMarkus Fendt, Thomas Endres, and Raimund Apfelbach Tierphysiologie, Universität Tübingen, D-72076 Tübingen, Germany
ABSTRACT
TOP
ABSTRACT
Introduction
Presentation of trimethylthiazoline (TMT, a component of fox feces) to laboratory rats elicits freezing, a prominent behavioral sign of anxiety or fear. The present study investigated the neural basis of this unlearned response. Muscimol, a GABAA receptor agonist, was injected (4.4 nmol/0.5 µl) into the bed nucleus of the stria terminalis (BNST) as well as into the amygdala, two brain areas known to be involved in anxiety and fear. Temporary inactivation of the BNST but not of the amygdala significantly blocked TMT-induced freezing. This effect was not caused by an enhancement of motor activity after BNST inactivation. In addition, these results confirm previous studies showing that freezing is possible despite amygdala inactivation. These results, and other findings in the literature, suggest that the BNST is critically involved in unlearned fear, whereas the amygdala is more involved in the acquisition and expression of learned fear.
Key words: amygdala; bed nucleus of the stria terminalis; fear; odor; muscimol; predator; temporary lesion
Introduction
Fear is a functional behavioral system that prepares an animal for a fast and effective hide, flight, or fight response in the presence of potentially dangerous environmental threats (Fanselow, 1991
; Fendt and Fanselow, 1999
One ecologically relevant signal that may elicit defensive behaviors, and fear, is the odor of a predator. Indeed, research with rats and mice has shown that fear is elicited by the odor of cats (Blanchard and Blanchard, 1989
Freezing is one of the most prominent behavioral symptoms of fear in rats (Griffith, 1920
Wallace and Rosen (2001)
The present study directly addressed this hypothesis. Specifically, we induced temporary lesions of the BNST or the amygdala by local microinjections of the GABAA receptor agonist muscimol and then measured TMT-induced freezing. In a post hoc experiment, possible effects of muscimol injections into the BNST on motor activity in an open field were investigated. This experiment was done to exclude the possibility that the observed effect of BNST inactivation in the main experiment was an artifact of the effects of muscimol on motor activity.
Materials and Methods
Subjects. Thirty-eight male Sprague Dawley rats (Charles River, Sulzfeld, Germany) weighing 220-260 gm at the time of the surgery were used. The animals were maintained on a 12 hr light/dark cycle, and food and water were available ad libitum. All experiments were performed in accordance with ethical guidelines for the use of animals in experiments and were approved by the local animal care committee (Regierungspräsidium Tübingen, ZP 5/99).
Surgery. Rats were anesthetized with ketamine/xylazine (9:1; 100 mg/kg, i.p.) and placed in a stereotaxic frame with blunt ear bars. Two stainless guide cannulas (diameter, 0.7 mm) were implanted bilaterally into the brain aiming at the BNST (0.5 mm rostral, ±1.4 mm lateral, 6.5 mm ventral to bregma) (Paxinos and Watson, 1997
Apparatus for odor exposure. Rats (n = 28) were placed in one of three identical exposure boxes (30 × 30 × 30 cm) made of polyvinyl chloride to assess TMT-elicited freezing. The front doors of these chambers were constructed of Plexiglas to permit observation of the rats. The behavior of the animals was recorded for later analyses.
Each exposure box was connected via Teflon tubing to a generator supplying charcoal filtered air; the outflow of the box was connected to an exhaust system. The air stream could be directed by electrically operated three-way Teflon valves either directly to the exposure boxes or through a glass bottle containing the odorant [20 µl of 2,4,5-trimethylthiazoline (PheroTech Inc., Delta, Canada) on a piece of filter paper] and then to the boxes. In both cases, clean air or air/odor flows were regulated with needle valves (17 l/min) and monitored by flow meters.
Procedure for odor exposure. To familiarize the rats with the olfactory exposure boxes, each animal was placed for 10 min into one of the exposure boxes (once per day on 5 consecutive days). On the following day, freezing behavior of the animals in the boxes was recorded during a 15 min period. After the fourth minute, the valve controlling the air flow was switched, but clean air (i.e., no TMT) was still presented to the animals on this first test day. On the next 2 d, each animal received (in a pseudorandomized manner) bilateral injections of either 4.4 nmol of muscimol [dissolved in 0.5 µl of artificial CSF (ACSF)] or ACSF alone into the BNST (n = 12) or amygdala (n = 13). The solutions were infused bilaterally at a rate of 0.1 µl/10 sec. After the injection, cannulas were left in place for another 2 min to allow diffusion of the solution away from the cannula. Previous research has shown that the injected drug diffuses in an area of ~1 mm diameter around the injection site with these sorts of parameters (Miserendino et al., 1990
Immediately after the infusions, animals were placed into the odor exposure boxes and were observed for 15 min. After 4 min, the Teflon valves were switched and TMT was directed into the exposure boxes. After this test, animals were placed into a cage located in a fume hood for 2 hr and then returned to their home cages. After each experimental session, the odor chamber, and tubing, was thoroughly washed with 70% ethanol and ventilated with clean air for 2 hr.
The videotapes from all experiments were analyzed by one observer who was not aware of the animal's condition. Freezing was used to measure fear. Freezing is characterized by crouching, with cessation of movements except those associated with breathing (cf. Blanchard and Blanchard, 1969
Motor activity in the open field. Motor activity of rats (n = 10) was measured in an open field made of gray plastic with a diameter of 80 cm (height of the walls, 25 cm). The open field was divided into 16 subfields. After injections (as above), each rat was placed in the center of the open field, and horizontal motor activity (line crossings of all four legs) was quantified over 15 min. Line crossings were evaluated on-line by an observer via a video camera.
Statistical analysis. Statistical analysis of the freezing data were accomplished by ANOVA (followed by post hoc Tukey tests). Motor activity data, for groups and across time, were analyzed by ANOVA and by t tests.
Results
Histology
The injection sites within the BNST and the amygdala are shown in Figure 1. For those rats tested for TMT-induced freezing, 12 injection sites were located in the BNST and 13 injection sites were located in the lateral nucleus of the amygdala. The data from three animals were excluded from analysis because of misplaced injection sites (hippocampus, putamen caudatus). For those rats tested for motor activity in the open field, all 10 injection sites were located in the BNST.
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Figure 1. Reconstructions of the different injection sites of ACSF and muscimol into the BNST (A, , test on TMT-induced freezing;
, test on motor activity) and amygdala (B). The coronal sections were taken from the atlas of Paxinos and Watson (1997)
TMT-induced freezing
Analysis of freezing during the first test day (clean air only) revealed no effects of group, time, or interaction (F values of <1.53). Levels of freezing were consistently low in this test (19.5-24.1%; data not shown).
ACSF-injected rats
To determine the effects of TMT on freezing, two sets of within-subjects analyses were done. In the first set, performance during odor presentation was compared with baseline performance. As in previous studies (Wallace and Rosen, 2000
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Figure 2. Time courses of the mean ± SEM percentage of time spent freezing to TMT in BNST-injected (circles) and amygdala-injected (diamonds) animals. The gray box at the bottom indicates the duration of TMT presentation.
To ensure that these increases in freezing to the odor were not merely attributable to the passage of time, a second set of analyses was done: Freezing during TMT presentation was significantly higher than freezing with clean air during the same time window of the test on the previous day (p values of <0.001).
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Figure 3. Mean ± SEM percentage of time spent freezing to TMT in the pre-odor (min 1-4) and post-odor (min 5-15) condition. **p < 0.01 compared with the pre-TMT condition; ++p < 0.01 compared with ACSF treatment (ANOVA followed by a post hoc Tukey test).
Injections of muscimol into the amygdala
To estimate the role of the amygdala and BNST in TMT-induced freezing, the freezing rates after muscimol injections were compared with those after ACSF injections. Muscimol injections into the amygdala did not affect TMT-induced freezing (Figs. 2, 3; interaction of drug and odor, F < 1.0). This was confirmed by post hoc comparison showing an increase in freezing rate during TMT presentation (p < 0.001).Injections of muscimol into the BNST
In contrast, muscimol injected into the BNST blocked the increase in freezing elicited by TMT (Figs. 2, 3; interaction of drug and odor: F(1,30) = 4.98; p = 0.03). This was confirmed by a post hoc Tukey test showing no differences in freezing during the baseline period and during TMT presentation after muscimol injections into the BNST (p = 0.81). It is important to note that the baseline freezing response before TMT presentation was not affected by muscimol injections into either the amygdala or the BNST (post hoc Tukey tests: comparisons between ACSF and muscimol; p values >0.43).Motor activity in the open field
To ensure that the blockade of TMT-induced freezing after muscimol injections into the BNST was not caused by a simple enhancement of motor activity, we measured the effects of muscimol injections into the BNST on horizontal motor activity in the open field. The results showed that motor activity in the open field was not affected by muscimol injections into the BNST (Fig. 4; effect of drug and interaction drug × time: F values of <1.5; p values of <0.15). A comparison of the total motor activity collapsed over the 15 min test also failed to reveal a significant group difference (Student's t test; t = 0.28; p = 0.78).
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Figure 4. Time course of motor activity measured by line crossings ± SEM during a 15 min period in an open field. The rats received injections of ACSF ( ) or muscimol (
Discussion
The present study tested whether the BNST and the amygdala are involved in TMT-elicited freezing. Specifically, we temporarily inactivated the BNST and the amygdala by local microinjections of the GABAA receptor agonist muscimol and then measured TMT-induced freezing. Most importantly, the present study demonstrated a total disruption of TMT-induced freezing after temporary inactivation of the BNST but not of the amygdala. This effect was not attributable to an increase in motor activity after muscimol injections into the BNST.
TMT-induced freezing
In the present study, TMT induced a high rate of freezing. Similar results were reported by Wallace and Rosen (2000
A comparison of complete odors (e.g., via a cat collar) and individual components of an odor (e.g., TMT) should be done with caution. Furthermore, it should be noted that there were some methodological differences between the different cited studies: In all experiments, test chambers of similar sizes were used, but those used by McGregor et al. (2002)
Before TMT presentation, the animals in the present study showed a freezing rate between 20 and 40%. This is a higher rate than observed by Wallace and Rosen (2000)
Role of the amygdala in TMT-induced freezing
The present study clearly shows that temporary inactivation of the amygdala does not affect TMT-induced freezing. This supports the results of Wallace and Rosen (2001)
This finding might be seen as surprising given that the amygdala is one of the main neural structures involved in behavioral fear responses. Different studies have demonstrated that the amygdala, especially its lateral, basolateral, and central nuclei, is necessary for the acquisition and expression of conditioned fear (Davis et al., 1993
Both the anterior cortical and the medial nucleus of the amygdala are far away (>2 mm) from our injection sites, and it is questionable whether muscimol injected in the present study reached these nuclei. However, the ineffective injection sites into the dorsal part of the amygdala are closer to these nuclei than the effective injection sites into the BNST, so this provides a strong argument against the idea that the effect of muscimol within the BNST was caused by diffusion to these nuclei.
The present study investigated the role of the amygdala and the BNST in freezing elicited by an unlearned olfactory stimulus. Several recent studies have used an odor as a conditioned stimulus (CS) in a fear-conditioning paradigm (Otto et al., 1997
Role of the BNST in TMT-induced freezing
In the present study, temporary inactivation of the BNST completely blocked TMT-induced freezing. It is important to note that this blockade of freezing was not a side effect of muscimol injections into the BNST on motor activity. Our control experiment demonstrated no changes in motor activity after muscimol injections into the BNST for 15 min (the duration of the TMT tests). To the best of our knowledge, this is the first study showing that the BNST is involved in olfactory-induced fear behavior. Nevertheless, this finding is not surprising because (1) the BNST is strongly connected to the olfactory system (Shipley et al., 1995
Both the amygdala and the BNST have very similar afferent connections and projections to various brain regions known to be involved in behavioral and autonomic symptoms of fear and anxiety (Davis and Shi, 1999
Conclusion
In summary, we demonstrated that TMT, a component of fox feces, is able to elicit freezing in rats, and that the TMT-induced freezing response can be blocked by temporary inactivation of the BNST but not of the amygdala. These results confirm the hypothesis that the BNST is important for the mediation of unlearned fear responses, whereas the amygdala is more involved in the learning of fear and in responses to conditioned stimuli.
FOOTNOTES Received July 24, 2002; revised Oct. 8, 2002; accepted Oct. 22, 2002.
This research was supported by Deutsche Forschungsgemeinschaft Grant SFB 550/C8. We are grateful to Christine Buck and David Hamm for their help in collecting the data, Helga Zillus for excellent technical assistance, and Dr. Rick Richardson for helpful comments regarding this manuscript.
Correspondence should be addressed to Dr. Markus Fendt, Tierphysiologie, Universität Tübingen, Auf der Morgenstelle 28, D-72076 Tübingen, Germany. E-mail: markus.fendt{at}uni-tuebingen.de.
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