Hemodynamic response pattern predicts susceptibility to stress-induced elevation in arterial pressure in the rat

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Hemodynamic response pattern predicts susceptibility to stress-induced elevation in arterial pressure in the rat

Jay R. Muller, Khoi M. Le, William R. Haines, Qi Gan, and Mark M. Knuepfer

Department of Pharmacological and Physiological Science, Saint Louis University School of Medicine, Saint Louis, Missouri 63104

ABSTRACT

TOP
ABSTRACT
INTRODUCTION
METHODS
RESULTS
DISCUSSION
REFERENCES

Cocaine or air jet stress evokes pressor responses due to either a large increase in systemic vascular resistance (vascularresponders) or small increases in both cardiac output and vascularresistance (mixed responders) in conscious rats. Repeated cocaineadministration results in elevated arterial pressure in vascularresponders but not in mixed responders. The present study examinedthe hypothesis that the pattern of cardiovascular responses toan unconditioned stimulus (UCS; air jet) is related to responsesto a conditioned stimulus (CS; tone followed by brief foot shock)in individual rats. Our data demonstrate that presentation ofthe UCS produced variable cardiac output responses that correlatedwith responses to the CS (n = 60). We also determined whetherindividual cardiovascular response patterns to acute stress correlatedwith predisposition to a sustained stress-induced elevation inarterial pressure. Rats were exposed to three different stressorspresented one per day successively for 4 wk and during a poststressperiod of 3 wk while arterial pressure was recorded periodically.Mean arterial pressure was elevated in all rats during chronicstress but, during the poststress period, remained at significantlyhigher levels in vascular responders but not mixed responders.Therefore, we conclude that acute behavioral stress to a conditionedstimulus elicits variable hemodynamic responses that predict thepredisposition to a sustained stress-induced elevation in arterialpressure.

behavioral stress; cardiac output; systemic vascular resistance

	INTRODUCTION

TOP ABSTRACT INTRODUCTION METHODS RESULTS DISCUSSION REFERENCES

THE ACUTE PRESSOR RESPONSE to mental arithmetic stress in humans is mediated either by an increase in cardiac output (CO)or an increase in systemic vascular resistance in most humans(6, 19, 22). Because of the response characteristics, theseindividuals have been referred to as cardiac and vascular responders,respectively (11, 25, 36, 47, 48). Several authors proposedthat autonomic responsiveness to behavioral stress in individualsis determined primarily by genetic factors (9, 24). Othershave suggested that hemodynamic reactivity to stress is predictiveof which individuals will develop hypertension (19, 32, 47,48). As yet, no longitudinal studies have linked greater vascularresponsiveness in humans with the development of hypertension.However, many investigators have reported that this variable isassociated with a predisposition to developing hypertension orwith a family history of hypertension (9, 10, 35-37). Theorigins of variable hemodynamic responsiveness and its relationshipto the development of hypertension are poorly understood, in partdue to the lack of a good experimental model. Although severalinvestigators have described models of stress-induced hypertensionin animals (20, 23, 31, 45), these models typically requirehyperresponsive strains or prolonged exposure to stress. No studiesto date, however, have explored vascular reactivity to stressas a predictor for susceptibility to stress-induced elevationsin arterial pressure in an animalmodel.

Branch and Knuepfer (4) noted hemodynamic responses in rats after administration of cocaine that were similar to thoseseen in humans exposed to stress. They demonstrated that cocaineelicited an acute increase in arterial pressure, which, in a subsetof rats termed vascular responders, was due to a large increasein systemic vascular resistance. A second group, named mixed responders,had identical pressor responses that were mediated by an increasein both CO and a smaller increase in systemic vascular resistance.Further studies revealed that air jet stress [unconditioned stimulus(UCS)] also caused variable hemodynamic responsiveness relatedto those evoked by cocaine in rats (27). The pressor responseto air jet was similar in vascular and mixed responders, whereasCO responses varied greatly. Vascular responders but not mixedresponders developed elevations in arterial pressure with repeatedadministration of cocaine (5). It is not known whether thefactors that determine acute response characteristics to stressor cocaine are related and correlate with the susceptibility todevelop sustained stress-induced hypertension (30).

The current study was designed to examine two hypotheses. First, we predicted that variable hemodynamic responsivity to anUCS (air jet) correlates with hemodynamic responses to a conditionedstimulus (CS; hemodynamic response to a 15-s tone preceding abrief foot shock). Second, we expected that hemodynamic responsevariability would be related to the predisposition to developstress-induced sustained elevations in arterial pressure suchthat repeated stress would elicit greater increases in arterialpressure in vascular responders compared with mixedresponders.

	METHODS

TOP ABSTRACT INTRODUCTION METHODS RESULTS DISCUSSION REFERENCES

Instrumentation. All surgical and experimental procedures were approved by the St. Louis University Institutional Animal Care and Use Committeeand followed guidelines described in the Guide for the Care andUse of Laboratory Animals [DHEW Publication No.(NIH) 85-23, Revised1996, Office of Science and Health Reports, DRR/NIH, Bethesda,MD 20205]. With an aseptic technique, male Sprague-Dawley rats(250-400 g, Harlan Sprague Dawley, Indianapolis, IN) were instrumentedwith a pulsed Doppler flow probe around the ascending aorta tomeasure ascending aortic blood flow and a femoral catheter todetermine arterial pressure and heart rate as described previously(4). Briefly, in rats anesthetized with pentobarbital sodium(45 mg/kg ip), a miniaturized pulsed Doppler probe was placedsnugly around the ascending aorta via a midline thoracotomy usingaseptic technique. The 36-gauge insulated leads were tunneledsubcutaneously to the skull, where a miniature electrical socketwas mounted using dentaladhesive.

After 7 to 10 days, rats were reanesthetized (using methoxyflurane) and a sterile catheter was implanted into the femoralartery for recording arterial pressure and heart rate. The COwas estimated using a directional pulsed Doppler flowmeter (Departmentof Bioengineering, University of Iowa). The flowmeter employeda 20-MHz incident signal with a 100-kHz sampling rate and antialiasingand autotracking circuits to reduce the incidence of unstableflow signals. In addition, all pulsatile flow signals were monitoredcontinuously on an oscilloscope to verify the absence of changesin waveform. If abrupt changes were noted, the data werediscarded.

Arterial pressure, heart rate, and ascending aortic blood flow in freely moving rats were recorded on a chart recorder. Changesin ascending aortic blood flow were used to estimate changes inCO. The change in systemic vascular resistance was calculatedby dividing arterial pressure by the CO while the change in strokevolume was determined by dividing the CO by the heart rate. Ratepressure product was calculated by multiplying heart rate by arterialpressure. These calculations have been used to estimate hemodynamicparameters in previous studies (4, 5, 27).

Acute stress. Reactivity in individual rats was tested with an UCS (air jet) and a CS (tone followed by a brief foot shock). One day afterarterial catheters were implanted, rats were acclimated to a Plexiglasand stainless steel test cage (25 × 30 × 30-cm, BRS/LVE, Laurel,MD) for 6 h. On the following day, rats were acclimated to thesame cage for 1-2 h after a small diameter (1.77 mm ID) polyethylenetube (PE-260, Clay Adams, Parsippany, NJ) was attached to thecable connected to the socket on the skull to deliver air puffsat a distance of 10-12 mm to the face of the rat. After acclimation,six trials of a brief (1-2 s) puff of air (1.4 kg/cm²) were administered at ~10-min intervals. After the six air jettrials, the animal was subjected to 12 trials of a 15-s tone (85-90dB) followed by a half-second shock via the test cage floor grid.The shock intensity was adjusted for each rat to elicit a flinchbut not vocalization. This paradigm is similar to that describedby Randall and coworkers (43). All measurements were taken within5 s after the initiation of the tone before the ensuing foot shock.The initial response to the CS, described as the C1 response byRandall et al. (43), was recorded. Three to five days later,rats were exposed to a chronic stressprocedure.

Chronic stress. To identify individual rats sensitive to sustained stress-induced increases in arterial pressure, we used three differentstressors presented on successive days such that the animal wasexposed to stressors six days a week for 4 wk. The stressors includedcold water stress in which the animal was placed in a plasticcage before adding 1 cm of cold (4-6°C) water. The water was keptat this temperature for the entire 1-h cold stress period. Onthe following day, restraint stress was used in which the animalwas immobilized in a plastic tube for a period of 1 h. Finally,on the third day the rat received 36 paired tone-shock stimuliat 5-min intervals as previously described. This series of dailystressors was repeated seven more times such that each rat receivedthree different stressors eight times over a 4-wk period. Arterialpressure was measured immediately before each stress period wheneverpossible. After the chronic stress period, we recorded mean arterialpressure for 3 wk, taking six measurements over a 1-h period aftera 1-h acclimation period 3-6 days/wk. Due to the prolonged experimentalperiod, all animals were recannulated (using the right femoralartery) 2-4 days before the end of the 4-wk stress period to ensureaccurate arterial pressurerecordings.

Control animals. Eight rats were used as control subjects. Although all were cannulated for arterial pressure measurement, only five of eightwere instrumented for CO determination. All animals were exposedto the acute stress paradigm (6 air jets and 12 tone-shock combinations)initially, then brought from the animal housing area to the labdaily for the 7 wk but not exposed to the stressors describedabove.

Euthanasia and histologic techniques. Animals were euthanized with pentobarbital sodium (70 mg/kg ip) after completion of the chronic stress paradigm. The heartswere fixed in formalin, sectioned, and stained with hematoxylinand eosin using standard techniques (26). An individual unfamiliarwith the treatment and response characteristics of each rat examinedthe tissue via lightmicroscopy.

Data analysis. The hemodynamic responses to the first three tone presentations were analyzed but not used to calculate the mean responses,because animals had to learn that the tone preceded the foot shock.Therefore, the responses to the six UCS and fourth through twelfthCS presentations during the acute stress period were summarizedand averaged for each individual rat. With the use of CO responses,the rats were then classified as vascular or mixed responders,in a manner similar to that previously described in our laboratory(27), to facilitate the analysis of possible differences betweenanimals at either end of the population distribution. Vascularresponders had a consistent change in CO of $<=$ 5% increase afterexposure to the CS. Alternatively, rats with CO responses >5%to CS were considered mixed responders. The CO responses to acuteair jet were used in a similar manner with a cutoff of 2% changeto define vascular and mixed responders to unconditioned stressfor Table 1 and Fig. 1. The cutoff values were derived by examiningthe response distribution depicted in RESULTS (Fig. 1). The cutoffvalues represented convenient points for separation of a primarypeak from a skewed tail. The responses to the conditioned stresswere less likely to change with repeated exposure and were, therefore,used to define vascular and mixed responders.

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Table 1. Cardiovascular Responses to UCS and CS

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Fig. 1. Distribution of mean cardiac output (CO) responses in individual rats to the unconditioned stimulus (UCS; A; air jet, 6 trials) and a conditioned stimulus (CS; B; tone, 9 trials) obtained at the time of the peak pressor response showing the distinction between vascular (hatched bars) and mixed (solid bars) responders. The cutoff values for separating groups were determined arbitrarily as shown. Insets: values from those rats that were exposed to the chronic stress paradigm.

To characterize rats, hemodynamic responses at the time of peak pressure response to acute stress were analyzed using an unpairedStudent's t-test (separate variances). Arterial pressure onlywas measured during the chronic stress period and analyzed usingan analysis of variance with repeated measures and Bonferroni'spost hoc comparison of differences at individual time points.In addition, simple regression analysis was performed to compareCO responses and changes in arterial pressure. All statisticalanalyses were performed using GB-STAT (Dynamic Microsystems, SilverSpring, MD). The data are expressed as the means ± SE, and differenceswere considered significant if P < 0.05.

	RESULTS

TOP ABSTRACT INTRODUCTION METHODS RESULTS DISCUSSION REFERENCES

Comparison of responses to UCS and CS. Rats (n = 60) were tested to compare hemodynamic responses to an UCS with those to a CS. Resting values for hemodynamic parametersare shown in Table 1. Within 5 s, the CS evoked a substantialincrease in arterial pressure, heart rate, and variable increasesin CO, systemic vascular resistance, and stroke volume (Table1). The UCS elicited similar responses to the CS, including increasesin arterial pressure, heart rate, CO, and systemic vascular resistanceand a variable change in stroke volume that occurred within 1-2s (Table 1).

Rats were divided into two groups according to the CO responses to the UCS and CS as previously described for responses tococaine and to air jet (5, 4, 27). The distributions ofthe CO responses to air jet (UCS) and to tone preceding shock(CS) are shown in Fig. 1. The distributions resembled a modalpeak with a skewed tail. We arbitrarily separated the peak fromthe skewed tail to analyze possible differences in susceptibilityto sustained stress-induced increases in arterialpressure.

There was a direct correlation (as determined by linear regression) between the magnitude of the CO responses to the UCS andto the CS (r = 0.67, P < 0.0001, Fig. 2). There was no correlationfor arterial pressure or heart rate responses to the CS and UCS(data not shown). There were significant differences in the CO,systemic vascular resistance, and stroke volume responses to theUCS and CS but not to the arterial pressure or heart rate changes(Table 1). Vascular responders had an elevated arterial pressurecompared with mixed responders before the initial UCS testingperiod. There were no differences in the resting heart rate orCO in these groups.

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Fig. 2. Variable CO response elicited by an UCS compared with that elicited by a CS using linear regression. There was a significant correlation between the measures (r = $-$ 0.67, P < 0.0001). Vascular responders to the CS (

) are differentiated from mixed responders ( $open circle$ ).

Repeated administration of the UCS produced progressively smaller pressor responses, although the profile of the responseswere not different in mixed responders compared with vascularresponders (Fig. 3). In contrast, the pressor and cardiac outputresponses to the CS were relatively consistent over repeated trialsafter the first two to three trials (Fig. 3). We ascribed thisto the training required for conditioning and omitted the firstthree trials from the calculations used to classify rats as vascularor mixed responders to a conditioned stressor. Data obtained forthe CS were virtually identical on the second day and are notdepicted in Fig. 3. Because of the reduced variability of thehemodynamic responses to the CS compared with the UCS, responsesto the CS were used to classify rats as vascular or mixed respondersduring chronic stress. Rats were allowed to recover for 3-5 daysbefore beginning the chronic stress paradigm.

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Fig. 3. The effects of repeated exposure to an UCS (A) and a CS (B) on mean arterial pressure (MAP) and CO responses at the time of the peak pressor response. As mentioned, additional trials with UCS were not performed due to the apparent acclimation (note reduced pressor and CO responses after repeated UCS). An analysis of variance with repeated measures was performed on the data to determine differences between mixed responders ( $open circle$ ) and vascular responders (

). *Significant differences between these groups (P < 0.05). Responses to the UCS represent data obtained on 2 successive days, whereas only the 1st day of the CS data is depicted.

Effects of chronic stress. Although most of the rats tested for acute hemodynamic responsiveness to stress were exposed to chronic stress, data fromonly 29 rats were compared during the 4-wk stress period and the3-wk recovery period. The remaining rats were omitted becausethey had <3 wk total of arterial pressure data (pre- and poststressperiods) or had no poststress data due to obstructed cannulas.The distribution of CO responses from rats used for the chronicstudy are depicted in Fig. 1, insets, to provide a comparisonto the larger population used to compare responsiveness. Again,data at some time points (primarily week 3 of the stress periodand the recovery or poststress period) were not available fromall rats due to blocked arterial cannulas. The hemodynamic responsesfrom the stress period were not different from those data obtainedin the initial comparison of responses to the UCS and CS. Forall subsequent analyses, animals were characterized as vascularand mixed responders according to their response to theCS.

Although the hemodynamic responses to repeated stress were not recorded during the 4-wk stress paradigm and the subsequent3-wk recovery period, arterial pressure was recorded several timesa week before exposure to the daily stressor after a 1- to 2-hacclimation period whenever arterial catheters remained patent.The changes in arterial pressures were averaged weekly in vascularand mixed responders and are depicted in Fig. 4. Repeated stresselicited a significant increase in arterial pressure in all animalsover the 4-wk stress period [P < 0.0004, F = 6.8, degrees of freedom(df) = 3,87, significant interaction = 0.033], although therewere no differences between vascular and mixed responders duringstress (P = 0.42, F = 0.68, df = 1,87). In contrast, during theentire 7-wk study, vascular responders had significantly greaterincreases in arterial pressure compared with mixed responders(P = 0.025, F = 5.6, df = 1,174). The difference in arterial pressurewas dependent on the changes during the 3 wk after the stresspresentation, which were significantly greater in vascular responders(P < 0.0001, F = 22.3, df = 1,58). During this same period, therewas no significant change in arterial pressure in eight controlanimals (Fig. 4).

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Fig. 4. The effects of chronic behavioral stress on mean arterial pressure (MAP) in mixed responders ( $open circle$ ), vascular responders (

), and unstressed rats ( $triangle$ ). Data were analyzed by analysis of variance with repeated measures and Bonferroni's post hoc comparisons. Repeated stress elicited a significant increase in the change in MAP in both groups of rats over the 4-wk stress period (W1-W4; P = 0.0004), although vascular and mixed responders were not different (P = 0.42). In contrast, the change in arterial pressure remained elevated only in vascular responders during the 3-wk poststress period (P1-P3) compared with baseline (P < 0.0001). Vascular responders had significantly greater increases in arterial pressure at 2 and 3 wk after stress compared with mixed responders using Bonferroni's post hoc procedure. The values in parentheses represent the n value at each data point. n values varied because of occasional loss of the arterial pressure signal. *Significant differences between groups (P < 0.05).

Histologic analysis of the hearts from individual rats revealed few abnormalities in either of the groups. In seven cases,a mild to moderate epicarditis was noted. This change has beennoted by our laboratory in previous studies (26) and is likelyto be due to alterations induced by damage to the epicardial sacduring surgery to implant the aortic flowprobe.

	DISCUSSION

TOP ABSTRACT INTRODUCTION METHODS RESULTS DISCUSSION REFERENCES

The present results suggest that chronic exposure to stressors causes sustained elevation in arterial pressure in a subsetof rats. Susceptibility to sustained stress-induced hypertensionis directly correlated with the hemodynamic response profile,particularly the relative contribution of CO and systemic vascularresistance to the pressor response. Variable CO responsivenessto stress has also been noted in humans (19, 32, 47, 48).Recent evidence has suggested that those individuals whose responseto stress is primarily due to an increase in total peripheralresistance (similar to our subgroup of vascular responders) havea greater predisposition to developing hypertension or have afamily history of hypertension (9, 10, 35-37) and are at greaterrisk of heart disease (12). The use of vascular reactivity asa risk factor for determining the development of hypertensionhas not been used in any longitudinal human studies. It has beensuggested, however, that this may be a risk factor in the African-Americanpopulation, who have both a greater propensity to develop hypertensionand greater vascular reactivity to cold stress (14).

We previously demonstrated that cocaine elicited similar hemodynamic responsiveness to air jet stress in rats (27). Branchand Knuepfer (5) reported that cocaine administration twicedaily for 5 days caused a sustained increase (measured on thefollowing day) in arterial pressure in vascular responders butnot in mixed responders. Therefore, we hypothesized that behavioralstress would produce a greater increase in resting arterial pressurein vascular responders compared with mixed responders after exposureto chronic stress. The present results support this hypothesis.Therefore, it is possible that the rat may provide a model tounderstand the causes of variable responsiveness and susceptibilityto sustained stress-inducedhypertension.

Several models have been developed to study the causes of stress-induced hypertension. These models have typically been limitedto special strains of rats (1, 31), to surgical interventions(3), or to prolonged exposure to behavioral stress (7, 15,20, 23). The present model uses outbred Sprague-Dawley rats,a strain not known for its sensitivity to stress-induced hypertension.In previous studies from our laboratory, highly variable hemodynamicresponsiveness to cocaine and to air jet stress were also observedin inbred Brown Norway and Fisher strains (unpublished data).Therefore, the varying responsiveness is not likely to be uniqueto this strain or this species. We propose that this may be aviable model to study the causes of sustained stress-induced increasesin arterial pressure that does not require a hypersensitive strainof rat or prolonged exposure to behavioral stress (29, 30).Although our model did not produce severe hypertension, it wasrelatively limited in the extent of exposure to behavioral stress.Nonetheless, the data suggest a sustained effect on arterial pressureregulation in a subset ofrats.

It is likely that previous studies required more prolonged stress because they were using a population of rats both susceptibleand resistant to stress-induced hypertension. Indeed, severalinvestigators describe the development of hypertension in somebut not all subjects exposed to stress using rats (1, 15,38) or monkeys (16, 21). We suggest that susceptible individualsmay have characteristic hemodynamic responses to stress, althoughresting values may not be predictive of the propensity to develophypertension (42).

The overall increase in arterial pressure elicited by the chronic stress paradigm was modest compared with the levels of hypertensionnoted in hypertensive humans or rats (3, 34, 40, 44).Most studies examining stress-induced hypertension have notedincreases of pressure of 10-20 mmHg, similar to the current study(1, 15, 16, 21, 38). It is likely the greater increasesin arterial pressure noted in hypertensive humans is due to thelonger duration of its development (e.g., 10-20 yr). This is moredifficult to simulate feasibly in animal studies without selectingspecific genetic factors that predispose individuals to develophypertension.

Several studies proposed that hypertensive patients or those likely to develop hypertension (due to family history) had greaterincreases in blood pressure than normotensive patients (14,17, 22, 36, 46). In the present study, there was no correlationbetween blood pressure or heart rate responsiveness to acute stressand predisposition to chronic stress-induced increases in arterialpressure. Therefore, it is likely that this strain of rat is nota useful model for studying thesephenomena.

The variable responsiveness noted actually represents a continuum of hemodynamic responses. As noted in Fig. 1, the animalsare arbitrarily grouped into mixed and vascular responders tocreate two groups and facilitate statistical comparisons of animalsat either end of a wide distribution. Further examination, particularlyof the extreme examples in this population may provide additionalinformation regarding the causes of predisposition tohypertension.

Our results also suggest that the acute hemodynamic responses evoked by an UCS are directly related to responses elicitedby a CS. Therefore, the type of stress may be less important thanthe individual responsiveness to the stressors. Indeed, our laboratorypreviously reported that cocaine evoked variable CO responsesthat were similar to those elicited by air jet (27). In fact,we noted variable CO responsiveness to a number of psychoactiveagents, including amphetamine, ethanol, bromocriptine, and desipramine(5, 28, 39). These data underscore the "universal" natureof the hemodynamic response pattern evoked by a number of disparatestimuli. This is not to say that all stressors evoke similar responses,because the pattern of hormonal responses to various stressorsdoes not support a consistent pattern (41).

The pressor response to an UCS diminishes with repeated exposure presumably due to acclimation. For this reason, we suggestthat the CS elicits a more consistent response pattern in individualrats and used this response as a more reliable indication of theindividual responsepattern.

The histologic changes noted using light microscopy were minimal and likely to be a result of surgical implantation of theDoppler flow probe. Our laboratory has noted accentuated developmentof myocardial injury in vascular responders compared with mixedresponders when exposed to cocaine using electron microscopy butnot light microscopy (26). Therefore, we suggest that highermagnification and more detailed analysis may be required to ascertainwhether myocardial injury is induced during the chronic stressparadigm.

In summary, acute pressor responses to a variety of stimuli are mediated by at least two mechanisms both in human and ratpopulations. Furthermore, this variable responsiveness can beused to predict sensitivity to cocaine-induced increases in arterialpressure in rats (5). An UCS can produce a similar variableacute increase; however, the pressor response diminishes withrepeated exposure. The results of these experiments indicate thata CS such as the tone-shock paradigm can produce a variable acuteincrease similar to that seen with the UCS (air jet), yet thepressor response does not diminish over time. Finally, the hemodynamicresponse pattern to behavioral stress (CS) can be used to predictthe predisposition to the development of sustained stress-inducedelevation in arterialpressure.

Perspectives

At present, it is unclear whether the differences in responsiveness and predisposition to elevated arterial pressure are dueto underlying genetic differences, although we recently suggestedthis hypothesis (30). In humans, differences in sensitivityto hypertension are likely to be determined by genetic factors,because individuals with a vascular response are more predominantin African-American men compared with Caucasian men (8, 33,44) and in men compared with women (2, 18). Vascular responsivenesshas been associated with a predisposition toward the developmentof hypertension, because both men and African-Americans are athigher risk for developing hypertension. Therefore, we proposethat the model of response variability may allow us to examinethe causes of differential responsiveness and predisposition tocardiovascular disease in an animal model. This may not only leadto new treatments but may be helpful in defining new risk factorsfor cardiovascular disease. Any additional information to improveclinical identification of susceptibility to cardiovascular diseasewould be expected to significantly improve diagnostic capabilityand improve healthcare.

	ACKNOWLEDGEMENTS

The authors thank Dr. J. Lemker for assistance in designing the stress paradigm and Dr. V. W. Fischer for assistance withthe histologicexaminations.

	FOOTNOTES

Portions of this work were published in abstract form (Haines WR, Muller JR, Gan Q, Lemker J, and Knuepfer MM. FASEB J 10:A629, 1996). We reported preliminary findings describing someof these data in previous reviews (29).

This work was supported by National Institutes of Health Grant DA-05180.

Address for reprint requests and other correspondence: M. M. Knuepfer, Dept. of Pharmacological and Physiological Science,Saint Louis Univ. School of Medicine, 1402 S. Grand Boulevard,St. Louis, MO 63104 (E-mail: knuepfmm{at}slu.edu).

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

Received 2 October 2000; accepted in final form 27 February 2001.

	REFERENCES

TOP ABSTRACT INTRODUCTION METHODS RESULTS DISCUSSION REFERENCES

1. Alexander, N. Psychosocial hypertension in members of a Wistar rat colony. Proc Soc Exp Biol Med 146: 163-169, 1974[Medline].

2. Allen, MT, Stoney CM, Owens JF, and Matthews KA. Hemodynamic adjustments to laboratory stress: the influence of gender and personality. Psychosom Med 55: 505-517, 1993[Abstract/Free Full Text].

3. Bernardis, LL, and Skelton FR. Effect of crowding on hypertension and growth in rats bearing regenerating adrenals. Proc Soc Exp Biol Med 113: 952-954, 1963.

4. Branch, CA, and Knuepfer MM. Dichotomous cardiac and systemic vascular resistance responses to cocaine in conscious rats. Life Sci 52: 85-93, 1993[ISI][Medline].

5. Branch, CA, and Knuepfer MM. Causes of differential cardiovascular sensitivity to cocaine I: studies in conscious rats. J Pharmacol Exp Ther 269: 674-683, 1994[Abstract/Free Full Text].

6. Brod, J. Haemodynamic basis of acute pressor reactions and hypertension. Br Heart J 25: 227-245, 1963.

7. Buckley, JP, Kato H, Kinnard WJ, Aceto MDG, and Estevez JM. Effects of reserpine and chlorpromazine on rats subjected to experimental stress. Psychopharmacologia 6: 87-95, 1964.

8. Calhoun, DA, and Oparil S. Racial differences in the pathogenesis of hypertension. Am J Med Sci 310, Suppl1: S86-S90, 1995.

9. Carroll, D, Hewitt JK, Last KA, Turner JR, and Sims J. A twin study of cardiac reactivity and its relationship to parental blood pressure. Physiol Behav 34: 103-106, 1985[Medline].

10. De Visser, DC, van Hooft IM, van Doornen LJ, Hofman A, Orlebeke JF, and Grobbee DE. Cardiovascular response to physical stress in offspring of hypertensive parents: Dutch hypertension and offspring study. J Hypertens 13: 901-908, 1995[ISI][Medline].

11. Eliot, RS. The dynamics of hypertension $---$ an overview: present practices, new possibilities, and new approaches. Am Heart J 116: 583-589, 1988[ISI][Medline].

12. Eliot, RS. Stress and the heart: mechanisms, measurement and management. Postgrad Med 92: 237-248, 1992.

13. Falkner, B. The role of cardiovascular reactivity as a mediator of hypertension in African Americans. Semin Nephrol 16: 117-125, 1996[ISI][Medline].

14. Falkner, B, Onesti G, Angelakos ET, Fernandes M, and Langman C. Cardiovascular response to mental stress in normal adolescents with hypertensive parents: hemodynamics and mental stress in adolescents. Hypertension 1: 23-30, 1979[Abstract/Free Full Text].

15. Farris, EJ, Yeakel EH, and Medoff HS. Development of hypertension in emotional gray Norway rats after air blasting. Am J Physiol 144: 331-333, 1945.

16. Forsyth, RP. Blood pressure responses to long-term avoidance schedules in the restrained rhesus monkey. Psychosom Med 31: 300-309, 1969[Abstract/Free Full Text].

17. Funkenstein, DH, King SH, and Drolette M. The direction of anger during a laboratory stress-induced situation. Psychosom Med 16: 404-413, 1954[Free Full Text].

18. Girdler, SS, Turner JR, Sherwood A, and Light KC. Gender differences in blood pressure control during a variety of behavioral stressors. Psychosom Med 52: 571-591, 1990[Abstract/Free Full Text].

19. Hejl, Z. Changes in cardiac output and peripheral resistance during simple stimuli influencing blood pressure. Cardiologia 31: 375-381, 1957[Medline].

20. Henry, JP, Meehan JP, and Stephens PM. The use of psychosocial stimuli to induce prolonged systolic hypertension in mice. Psychosom Med 29: 408-432, 1967[Abstract/Free Full Text].

21. Herd, JA, Morse WH, Kelleher RT, and Jones LG. Arterial hypertension in the squirrel monkey during behavioral experiments. Am J Physiol 217: 24-29, 1969.

22. Hickam, JB, Cargill WH, and Golden AC. Cardiovascular reactions to emotional stimuli: effect on the cardiac output, A-V oxygen difference, arterial pressure and peripheral resistance. J Clin Invest 27: 290-298, 1948.

23. Hudak, WJ, and Buckley JP. Production of hypertensive rats by experimental stress. J Pharm Sci 50: 263-264, 1961.

24. Jost, H, and Sontag LW. The genetic factor in autonomic nervous system function. Psychosom Med 6: 308-310, 1944[Abstract/Free Full Text].

25. Kasprowicz, AL, Manuck SB, Malkoff SB, and Krantz DS. Individual differences in behaviorally evoked cardiovascular response: temporal stability and hemodynamic patterning. Psychophysiology 27: 605-619, 1990[ISI][Medline].

26. Knuepfer, MM, Branch CA, Gan Q, and Fischer VW. Cocaine-induced myocardial ultrastructural alterations and cardiac output responses in rats. Exp Mol Pathol 59: 155-168, 1993[ISI][Medline].

27. Knuepfer, MM, Branch CA, Gan Q, and Mueller PJ. Stress and cocaine elicit similar cardiac output responses in individual rats. Am J Physiol Heart Circ Physiol 265: H779-H782, 1993[Abstract/Free Full Text].

28. Knuepfer, MM, and Gan Q. Effects of proposed treatments for cocaine addiction on hemodynamic responsiveness to cocaine in conscious rats. J Pharmacol Exp Ther 283: 592-603, 1997[Abstract/Free Full Text].

29. Knuepfer MM, Gan Q, Muller JR, Matuschak GM, and Lechner AJ. Hemodynamic response variability to behavioral stress correlates with predisposition to disease. In: Stress: Neural, Endocrine and Molecular Studies, edited by McCarty R, Aguilera G, Sabban E, and Kvetnansky R. In press.

30. Knuepfer, MM, and Mueller PJ. Review of evidence for a novel model of cocaine-induced cardiovascular toxicity. Pharmacol Biochem Behav 63: 489-500, 1999[ISI][Medline].

31. Lawler, JE, Barker GF, Hubbard JW, and Schaub RG. Effects of stress on blood pressure and cardiac pathology in rats with borderline hypertension. Hypertension 3: 496-505, 1981[Abstract/Free Full Text].

32. Light, KC, Dolan CA, Davis MR, and Sherwood A. Cardiovascular responses to an active coping challenge as predictors of blood pressure patterns 10 to 15 years later. Psychosom Med 54: 217-230, 1992[Abstract/Free Full Text].

33. Light, KC, Turner RJ, Hinderliter AL, and Sherwood A. Race and gender comparisons: I. hemodynamic responses to a series of stressors. Health Psychol 12: 354-365, 1993[ISI][Medline].

34. Lund-Johansen, P. Twenty-year follow-up of hemodynamics in essential hypertension during rest and exercise. Hypertension 18, Suppl III]: III-54-III-61, 1991.

35. Manuck, SB, Kasprowicz AL, and Muldoon MF. Behaviorally-evoked cardiovascular reactivity and hypertension: conceptual issues and potential associations. Ann Behav Sci 125: 17-29, 1990.

36. Manuck, SB, Proietti JM, Rader SJ, and Poleforne JM. Parental hypertension, affect, and cardiovascular response to cognitive challenge. Psychosom Med 47: 189-200, 1985[Abstract/Free Full Text].

37. Marrero, AF, al'Absi M, Pincomb GA, and Lovallo WR. Men at risk for hypertension show elevated vascular resistance at rest and during mental stress. Int J Psychophysiol 25: 185-192, 1997[ISI][Medline].

38. Medoff, HS, and Bongiovanni AM. Blood pressure in rats subjected to audiogenic stimulation. Am J Physiol 143: 300-305, 1945.

39. Mueller, PJ, Gan Q, and Knuepfer MM. Ethanol alters hemodynamic responses to cocaine in rats. Drug Alcohol Depend 48: 17-24, 1997[ISI][Medline].

40. Okamoto, K. Spontaneous hypertension in rats. Int Rev Exp Pathol 7: 227-270, 1969[Medline].

41. Pacek, K, Palkovits M, Yadid G, Kvetnansky R, Kopin IJ, and Goldstein DS. Heterogeneous neurochemical responses to different stressors: a test of Selye's doctrine of nonspecificity. Am J Physiol Regulatory Integrative Comp Physiol 275: R1247-R1255, 1998[Abstract/Free Full Text].

42. Post, WS, Larson MG, and Levy D. Hemodynamic predictors of incident hypertension: the Framingham heart study. Hypertension 24: 585-590, 1994[Abstract/Free Full Text].

43. Randall, DC, Brown DR, Brown LV, and Kilgore JM. Sympathetic nervous activity and arterial blood pressure control in conscious rat during rest and behavioral stress. Am J Physiol Regulatory Integrative Comp Physiol 267: R1241-R1249, 1994[Abstract/Free Full Text].

44. Saab, PG, Llabre MM, Hurwitz BE, Frame CA, Reineke LJ, Fins AI, McCalla J, Cieply LK, and Schneiderman N. Myocardial and peripheral vascular responses to behavioral challenges and their stability in black and white Americans. Psychophysiology 29: 384-397, 1992[ISI][Medline].

45. Sanders, BJ, and Lawler JE. The borderline hypertensive rat (BHR) as a model for environmentally-induced hypertension: a review and update. Neurosci Biobehav Rev 16: 207-217, 1992[ISI][Medline].

46. Stevenson, IP, Duncan CH, Flynn JT, and Wolf S. Hypertension as a reaction pattern to stress. Correlation of circulatory hemodynamics with changes in the attitude and emotional state. Am J Med Sci 224: 286-299, 1952.

47. Turner, JR. Cardiovascular Reactivity and Stress. NY: Plenum, 1994.

48. Turner, JR, Sherwood A, and Light KC. Individual Differences in Cardiovascular Response to Stress. NY: Plenum, 1992.

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