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NEUROHUMORAL CONTROL OF CARDIOVASCULAR FUNCTION

Differential acquisition of specific components of a classically conditioned arterial blood pressure response in rat

¹Department of Physiology, Faculty of Medicine, Suez Canal University, Ismailia, Egypt; and ²Department of Physiology, College of Medicine, and ³Center for Biomedical Engineering, University of Kentucky, Lexington, Kentucky

Submitted 11 January 2005 ; accepted in final form 26 April 2005

	ABSTRACT

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Presenting a 15-s pulsed tone, the conditional stimulus (CS⁺), followed by 0.5-s tail shock, to a well-trained rat causes a sudden, but transient, pressor response (C₁). Blood pressure (BP) then drops before increasing again (C₂). A steady tone of the same frequency never followed by a shock (a discriminative stimulus, or CS^–) evokes a C₁ but not a C₂ response. Experiment 1 tested the hypothesis that this BP response pattern does not depend on the nature of the tone (i.e., pulsed vs. steady) used for CS⁺ and CS^–. The tones were reversed from the traditional paradigm, above, in nine rats. The C₁ BP increase for a steady-tone CS⁺ (+4.8 ± 1.9 mmHg, mean change ± SE) and a pulsed CS^– (+2.9 ± 1.3 mmHg) did not differ. Conversely, C₂ showed a clear discrimination (CS⁺: +5.1 ± 1.2 mmHg, CS^–: +0 .7 ± 0.8 mmHg; P < 0.05). Experiment 2 tested the hypothesis that the C₁ and C₂ BP responses first appear at different times during training. On training day 1, five 15-s pulsed tones (CS⁺) were presented to each of 18 rats; the last tone was followed by a tail shock. Likewise, five steady CS^– tones never followed by shock were given. Training continued for 2 more days, with each CS⁺ followed by shock. At the end of day 2, CS⁺ evoked a C₁ BP response (+3.9 ± 0.9 mmHg) but no C₂ (+0.6 ± 0.4 mmHg, not significant vs. pretone). By the end of day 3, CS⁺ evoked a significant (vs. baseline) C₁ (+7.3 ± 1.4 mmHg) and C₂ (+3.3 ± 0.8 mmHg). Conversely, although CS^– evoked a C₁ response (3.5 ± 1.3 mmHg), there was no C₂ (+0.7 ± 0.5 mmHg; not significant). We conclude that 1) C₁ and C₂ are acquired at different rates, 2) early in training C₁ is an orienting response evoked by both tones, and 3) C₂ is only acquired as an animal learns to associate the CS⁺ tone with shock. This suggests that C₁ and C₂ are controlled by different processes in the brain.

Pavlovian conditioning; orienting response; habituation; learning

Recordings of renal sympathetic nerve activity (SNA) show why C₂ is a more definitive measure of discrimination. That is, the C₁ pressor response is preceded by a "sudden burst" in SNA (16), and the amplitude of the C₁ increase in BP is proportional to the transient but intense increase in SNA (2). We have suggested that C₁ is an open-loop response, probably resulting from a "central command" (16). During C₂, there are sustained but smaller magnitude increases in SNA during CS⁺ that do not occur in response to CS^–, making C₂ the more sensitive discriminator compared with C₁. Another important aspect of C₂ is that it appears to be under the control of the baroreflex (16).

We had previously assumed that the conditional changes in BP (C₁ and C₂) are in response to a perceived stress and not due to the differences in the quality of the tone itself. Experiment 1 tests the hypothesis that the pattern of the BP conditional response does not depend on the nature of the tone. All aspects of the conditioning were kept constant except that the solid tone was now followed by shock and the pulsed tone was used as the behavioral control. We found in fully trained subjects that the amplitude and pattern of the BP conditional response were the same in this "reverse tone" paradigm vs. our traditional procedure.

We also sought to determine the dynamics of the acquisition of C₁ compared with C₂. We hypothesized that the two appear at different times as the rat learns the conditioning paradigm. To accomplish this, we implanted an arterial catheter in untrained rats to measure BP before proceeding with 3 days of training in the discriminative conditioning paradigm. We found that 1) very early in training both tones evoked a short-latency BP increase that, with continued training, became the C₁ component; and 2) the C₂ component was acquired later in training; but 3) both components (i.e., C₁ and C₂) first showed discrimination between CS⁺ and CS^– at the same time (i.e., the end of the third training day). One attractive interpretation of these findings is that C₁ is initially part of an orienting response (OR) but, as the animal learns the paradigm, it comes under the control of the same central processes responsible for expression of the learned C₂. A preliminary account of these findings has been published (17).

	METHODS

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Subjects

Nine Sprague-Dawley rats (Harlan Industries, Indianapolis, IN) were used in the reverse tone experiment; eighteen Sprague-Dawley rats were used in the acquisition experiment. Rats weighed between 300 and 450 g at the time of data acquisition. The animals were maintained on standard rat chow and water ad libitum throughout the experiment, except during the time they were actively participating in the conditioning trials. The experimental protocol was approved by the University of Kentucky Animal Care and Use Committee.

Experiment 1: Reverse Tone Paradigm

Behavioral conditioning protocol. The animals were accustomed for 1 h daily over 2 days to handling and to restraint in a comfortable, conical cloth sock. Once adapted to the process, they typically remained quietly snuggled within the sock, although they were free to emerge; on such occasions, they were gently reintroduced to the restraint. Classical, or Pavlovian, conditioning traditionally requires that the CS⁺ and CS^– be initially neutral. Therefore, on the first day of training, each animal was habituated to the audio stimuli eventually to be used as the positive or reinforced tone (i.e., CS⁺) and the negative or nonreinforced tone (i.e., CS^–). Both tones were the same frequency (375 Hz) and length (15 s) and were 8 dB above background noise (66 dB); the only difference was that the CS⁺ tone was sounded continuously (i.e., steady), whereas the CS^– was regularly interrupted (i.e., pulsed: on for 0.064 s, off for 0.16 s). Five pairs of the pulsed and steady tones were presented to each rat in a pseudorandom sequence (e.g., CS^–, CS⁺, CS⁺, CS^–, etc.). A minimum of 4 min elapsed between trials. None of the tones for the first four sets was paired with shock during the habituation trials. The final (i.e., fifth) steady (i.e., CS⁺) tone was followed with a 0.5-s shock delivered between electrodes on opposite sides of the rat’s tail. The intensity of the shock was adjusted to the lowest value that caused the rat to flinch and vocalize ("squeak"); the intensity usually ranged between 0.2 and 0.3 mA and never exceeded 0.5 mA. Conditioning trials, in which each CS⁺ was always followed by tail shock, continued for the next 2 days. The pulsed CS^– tone was never followed by a shock. Five CS⁺ and five CS^– were given each day.

Surgery. After completion of training, above, the rats were anesthetized with pentobarbital sodium (65 mg/kg ip) in preparation for surgery. A Teflon arterial catheter (ID = 0.012 in.) was inserted into the upper abdominal aorta via the left femoral artery in six of the rats. The catheters were tunneled under the skin, exited at the nape of the animal’s neck, and run through a flexible spring tube to the top of the cage. A BP telemetry unit was implanted in three rats. The abdominal aorta was visualized via a laparotomy. The sensory element of a Data Sciences International probe (model TA11PA-C40) was placed into the aorta via a puncture such that the tip pointed toward the heart. The catheter containing the sensitive element of the probe was secured in place with surgical glue. The body of the probe was secured to the interior abdominal wall with sutures. The incision was closed, and the rat was monitored until it regained consciousness. The data were similar, regardless of how the pressure was measured, and were combined for analysis. The animal was returned to the cage and allowed to recuperate for 4 days before any experiment was performed.

Data acquisition and analysis. The rats were reintroduced to the restraint sock, as above, at the end of the recuperation period and tested in the conditioning paradigm for 2 days; five CS⁺ and five CS^– were given each day. BP was digitally sampled at 500 Hz using an analog-to-digital converter (Data Translation 2810) and a microprocessor. Data sampling began 9 s before onset of the tone and continued for 30 s (i.e., until 6 s after tone-off). The first 1 s of data was discarded. To utilize large data files, programs were developed for a 32-bit operating system (Windows NT) using Microsoft Visual C++ with foundation class. The digital files of the BP recordings during the 10 CS⁺ were ensemble averaged for each individual subject to yield a "high resolution" analysis of the conditional response for that rat (15, 16); likewise, the 10 CS^– trials were ensembled. The peak increase in mean BP (mBP) during C₁ and the average increase in mBP during C₁ (defined as the average value over the first 2 s of the tone) were determined for each rat from these ensembled data sets. The BP data between the 3rd and 5th s of the tone were skipped since they include the fall in pressure that separates C₁ from C₂ (15). Next, the average change in mBP during C₂ (defined as the average over the last 10 s of the tone) was measured for these same trials. All of the changes in mBP were measured relative to the average pressure during the pretone baseline control. Heart rate (HR) was determined from the pulsatile BP signal.

Experiment 2: Acquisition of Conditional Response Pattern

Behavioral conditioning protocol. Each rat was implanted with an arterial catheter and then allowed 4 days of recuperation. On day 1 of conditioning, five CS^– (solid tone) and five CS⁺ (pulsed tone) were given; however, only the last CS⁺ was reinforced by shock. On days 2 and 3 of conditioning, five tones of each type were presented with each CS⁺ followed by shock. On all 3 days of conditioning, data were collected during the first and the last trials for both CS⁺ and CS^–. The BP data were recorded for all conditioning trials starting with day 1 and extending through day 3. The peak and average C₁ and C₂ were recorded, as above, for the first and fifth trials each day.

Statistical analysis. The statistical significances of the changes in BP relative to baseline and of the differences between CS⁺ and CS^– responses were tested by ANOVA followed by post hoc Newman-Keul’s multiple range tests as allowed by a significant interaction in the ANOVA. Data are given as means ± SE. Statistical significance was accepted for P < 0.05.

	RESULTS

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Experiment 1

Figure 1 shows a composite analysis of mBP and HR across all nine rats trained in the reverse tone paradigm. Figure 1, top, was constructed by ensemble averaging the "high-resolution" BP files for CS⁺ trials across all animals. Note, therefore, that the conditional response for any individual animal was represented by a single data file. Likewise, Fig. 1, bottom, was constructed by ensembling the BP and HR data for the CS^– trials across rats. The tone began at 15 s and ended at 30 s (dark bar on x-axis). Note particularly in Fig. 1 the "classic" form of the BP conditional response with an obvious sudden but transient C₁ for each tone, a delayed, and smaller, C₂ pressor response for CS⁺ but not for CS^–. Finally, the shock that followed the CS⁺ evoked an unconditional increase in arterial pressure.

View larger version (20K): [in this window] [in a new window]   Fig. 1. Composite analyses over 9 rats of mean arterial blood pressure (mBP) and heart rate (HR) responses to all conditional stimuli (CS+; steady tone, top) and discriminative stimuli (CS–; pulsed tone, bottom) for experiment 1. Tones began at 15 s and terminated at 30 s. The 0.5-s tail shock was delivered between the 2 vertical lines (top). The C1 component of the conditional BP response is evoked by both CS+ and CS–. C2 is evoked only by CS+. This response pattern resembles that described previously (7, 13, 15, 16) when CS+ was a pulsed tone and CS– was a steady tone of the same frequency.

View larger version (11K): [in this window] [in a new window]   Fig. 2. A comparison between the average CS– and CS+ values for C1 and C2 in the reverse tone experiment. The C1 response is quantified as both its peak increase relative to baseline (left) and the average value over the first 2 s of the tone (middle); value for C2 (right) is the beat-by-beat average over the last 10 s of the tone. Note that the CS+ C2 is significantly larger than for CS–, demonstrating that the rats discriminated between tones in this "reverse" paradigm. oP < 0.05, compared with baseline. *P < 0.05, CS+ vs. CS–.

The standard pulsed tone for CS⁺ and steady tone for CS^– were used for experiment 2. Figure 3 presents means ± SE for the average increases in mBP for C₁ (i.e., over first 2 s of each tone) for CS⁺ and CS^– trials. Data are shown for the first and last (i.e., fifth) trials for each of the 3 days (e.g., day 1, tone 1 = D₁T₁; day 2, tone 5 = D₂T₅). Multivariate ANOVA [factors for CS⁺/CS^– and trials (D₁T₁... D₃T₅)] for repeated measures (subjects) confirmed significant interactions when tested for C₁ peak, C₁ average, and C₂ (F_5,85 = 2.66, 4.67, and 3.50, respectively). The average amplitude of the C₁ response significantly exceeded pretone baseline pressure the first time the animals heard the tone (D₁T₁) for both CS⁺ and CS^–; the two amplitudes did not differ. The size of the C₁ pressor response had decreased by trial D₁T₅ (not significant vs. baseline) as the animals habituated to the (nonreinforced) tones. C₁ was restored (P < 0.05 vs. baseline) by the sixth pairing of the tone and shock (i.e., the fifth tone on day 2: D₂T₅, Fig. 3), but the responses did not differ significantly between CS⁺ and CS^–. That is, the rats had not yet shown any discrimination between the two stimuli. Discrimination was achieved by D₃T₅. The findings with respect to the peak conditional change in BP for C₁ were similar; all increases were significant with respect to baseline, but, as with the average increase (Fig. 3), there was no demonstrable discrimination between tones until D₃T₅ (data not shown).

View larger version (13K): [in this window] [in a new window]   Fig. 3. Average amplitude of C1 component of conditional blood pressure response to CS+ (pulsed tone) and CS– (steady tone) for first (T1) and fifth (T5) presentation of tones for days 1–3 (D1, D2, D3). mBP was significantly increased over baseline control for all trials except the fifth CS+ and fifth CS– tones (T5) on day 1 and for the first CS+ on day 2 (D2T1). Increase in mBP to CS+ was not significantly greater than that to CS– until the fifth trial on day 3. *P < 0.05, CS+ vs. CS–.

View larger version (12K): [in this window] [in a new window]   Fig. 4. Average amplitude of C2 component of conditional blood pressure response to CS+ and CS– for first (T1) and fifth (T5) presentation of tones for days 1–3. Changes in mBP were not significantly increased over baseline control, except for the increase during CS+ for trial 5 (T5) on day 3. *P < 0.05, CS+ vs. CS–; oP < 0.05 compared with baseline.

	DISCUSSION

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In our previous work, we did not implant the arterial catheter until the subjects had been fully trained in the behavioral paradigm. Consequently, we had no information on the dynamics of the way in which the animals learned the conditional response. Our present demonstration that C₁ and C₂ are differentially acquired was possible because we were able to evaluate a given trial as the animals learned the paradigm (e.g., starting with the first tone on the first day of training: D₁T₁). The major findings of the acquisition study are that 1) there is an increase in BP similar in shape and timing to the C₁ component (i.e., as seen in the fully trained animal) in response to the first presentation of both the pulsed and steady tones (i.e., that become the CS⁺ and CS^–, respectively); 2) the first presentation of the tones evokes no significant increase in BP that corresponds in timing and magnitude to the C₂ conditional response; 3) as the animal is being trained in the conditioning paradigm, it expresses a short latency but transient pressor response (i.e., that eventually becomes the C₁ component of the conditional BP response) before the more latent, smaller pressor response (i.e., that becomes the C₂ component); and 4) the rats learn to discriminate between the tones relatively late in the training process. Note that, because both tones are the same frequency, the animals cannot know which tone is pulsed and which is steady for a few tenths of a second (i.e., the duration of a single pulse).

That different aspects of the conditional response can be acquired at different rates is not new. For example, conditional changes in BP, HR, respiration, pupil size, and the galvanic skin response are acquired more rapidly than conditional retractions of the nictitating membrane, eyelid, and flexion responses (reviewed in Ref. 11). To the best of our knowledge, however, the finding that different aspects of the conditional response for the same physiological variable, BP in our case, are acquired at a different rate is new. We believe that this study provides new insights into the autonomic control of arterial BP during acute behavioral challenges and that a careful examination of the nature of C₁ compared with C₂ provides interesting clues as to the explanation for this different rate of acquisition.

The classic view holds that the functional role of the OR is to intensify attentional processes to any new environmental stimulus. C₁ showed a number of features characteristic of an OR (reviewed in Ref. 1). First, it was evoked by the very first tone presentation and decreased in magnitude (habituated) with additional presentations of the nonreinforced tones (i.e., for both for CS⁺ and CS^–). Second, a pure OR to two similar tones would have comparable amplitudes, as was indeed the case for D₁T₁. However, there are also several pieces of evidence that C₁ is modified once the CS⁺ was reinforced. First, although the C₁ response decreased during the habituation phase, it started to increase in amplitude during day 2 in response to both tones. This increase in C₁ to both CS⁺ and CS^– in all probability reflects a generalization process: the animal had learned that a tone presages a shock but had not yet discriminated between CS⁺ and CS^–. By the end of day 3, however, C₁ was significantly larger for CS⁺ vs. CS^– trials, demonstrating that it, too, shows discrimination between tones (see also Refs. 13, 15, 16). We believe, therefore, that the pressor response for the trials during day 1 was a manifestation of an OR. By day 3, it had acquired characteristics of a learned response. If so, our data support the recent conclusion that the OR is "a complex polyfunctional activity, different aspects of which are reflected in different OR components that can be modified rather independently" (8).

The rate of extinction of the OR, and acquisition of the conditional response for different response systems, can differ significantly. With respect to the former, the autonomic components of the OR (HR, respiratory changes, and galvanic skin responses) habituate first followed by the EEG components (alpha desynchronization and vertex potential; Ref. 8). Latash (8) believed that this difference can be explained by different "habituation thresholds" in different brain systems. Powell (14) proposed that the differential acquisition represents different stages of the learning process, perhaps mediated within different regions of the brain. The evolution of the characteristics of C₁ from an OR to a learned response might be explained by a progressive shifting of the mediation of this initial response from one to another of the hypothesized brain regions.

In contrast to C₁, C₂ specifically appears to be acquired only as the animal learns the conditioning paradigm. Recall, for example, that a statistically significant C₂ had not appeared even by D₂T₅, probably because at least some of the rats had not yet learned the association between tone and shock. (This latter statement is also supported by the observation that there was no difference in the amplitudes of C₁ for the CS⁺ and CS^– tones throughout day 2.) By this logic, it was only during day 3 that the animals had learned the association between the CS⁺ tone and shock and could therefore discriminate between the reinforced CS⁺ and nonreinforced CS^–. This acquisition of a discriminative autonomic conditional response on day 3 was evidenced by 1) a significant difference in the C₁ response to CS⁺ vs. CS^– and 2) the emergence of a significant C₂ to the CS⁺ but not to the CS^–. We believe that these findings indicate that C₂ is attributable to central nervous processes directly indicative of associative learning.

A great deal is known about the role played by various parts of the central nervous system in the classical aversive conditioning of autonomic responses (reviewed in Ref. 9). It is widely accepted that the key neuronal systems receive information from both the conditional stimulus (i.e., the tone) and the unconditional stimulus (i.e., the shock). A great deal of experimental work has identified the amygdala as one of the critical centers for fear conditioning (e.g., Refs. 3, 9). Kapp et al. (6) were among the first to show, for example, that placing lesions within the central nucleus of the amygdala in the rabbit attenuates the conditional bradycardia. LeDoux et al. (10) placed lesions in regions of the rat brain to which the amygdala projected (lateral hypothalamic area, midbrain central gray, and bed nucleus of the stria terminalis); the animals were classically conditioned to shock 2 wk later. The lateral hypothalamic area lesions interfered with the conditional BP response but not the freezing response; conversely, the central gray lesions disrupted the conditional freezing but not the learned BP increase. In another important study, Gallagher et al. (4) showed that lesions placed in the central nucleus of the amygdala impaired acquisition of behaviors attributable to orienting-type responses; conversely, these animals did acquire conditional behavioral responses directly related to food delivery.

Perspectives

C₁ is undoubtedly a "complex polyfunctional activity" (8) that cannot be attributed to any single process. We have suggested that at least the initial portion of the C₁ response results from what we termed an open-loop relationship. For example, the sudden burst in SNA precedes the C₁ increase in BP (16), and preliminary findings indicate its amplitude is not significantly changed before vs. after sinoaortic denervation (18). We now propose that the initial, or rising phase, of C₁ is an OR, much like the sudden conditional tachycardia in dog (12). It is clear, however, that the peak amplitude of C₁ differs in CS⁺ vs. CS^– trials, so it can be modified by learning. C₁ is probably terminated by the baroreflex responding to the sharply elevated pressure (16). C₂ seems to be under the control of closed-loop biofeedback (i.e., baroreflex) mechanisms; in fact, our group (16) speculated that it may be due to an upward resetting of the baroreflex. These differences in the fundamental nature of the two components of the BP conditional response would be much easier to explain if C₁ and C₂ were mediated by different pathways within the nervous system. Moreover, this would make it easier to understand why C₁ appears to be less immediately reflective of actual associative learning processes than does C₂. Our recent finding (7) that chronic nicotine exposure depresses C₂ but not C₁ also appears to be in concert with the notion that the central mediation of these two components is fundamentally different. In any case, our finding that different components of the BP conditional response are acquired at different rates further extends the notion that classical conditioning is a complex, "polymodal" process (e.g., Ref. 5).

	GRANTS

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This work was supported by grants from the Kentucky Spinal Cord and Head Injury Research Trust (RB-9601-K3), the National Institutes of Health (HL-19343 and NS-39744), and the University of Kentucky Tobacco and Health Research Institute

	FOOTNOTES

 

Address for reprint requests and other correspondence: D. C. Randall, Dept. of Physiology, Univ. of Kentucky College of Medicine, Lexington, KY 40536-0298 (e-mail: randall{at}uky.edu)

The costs of publication of this article were defrayed in part by the payment of page charges. The article must therefore be hereby marked "advertisement" in accordance with 18 U.S.C. Section 1734 solely to indicate this fact.

	REFERENCES

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6. Kapp BS, Frysinger RC, Gallagher M, and Haselton JR. Amygdala central nucleus lesions: effect on heart rate conditioning in the rabbit. Physiol Behav 23: 1109–1117, 1979.[CrossRef][Medline]
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8. Latash LP. Orienting reaction, organizing for action, and emotional processes. Pavlovian J Biol Sci 25: 123–131, 1990.[Medline]
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18. Willingham A, Williams D, Brown L, Brown D, Cassis L, Silcox D, Anigbogu C, and Randall D. Arterial blood pressure response to an acute stress in rat following sino-aortic denervation (Abstract). FASEB J 18: A673–A674, 2004.

This Article Abstract Full Text (PDF) All Versions of this Article: 289/3/R784    most recent 00018.2005v1 Alert me when this article is cited Alert me if a correction is posted Citation Map Services Email this article to a friend Similar articles in this journal Similar articles in Web of Science Similar articles in PubMed Alert me to new issues of the journal Download to citation manager Citing Articles Citing Articles via Google Scholar Google Scholar Articles by El-Wazir, Y. M. Articles by Randall, D. C. Search for Related Content PubMed PubMed Citation Articles by El-Wazir, Y. M. Articles by Randall, D. C.