Lateralized Effects of Medial Prefrontal Cortex Lesions on Neuroendocrine and Autonomic Stress Responses in Rats

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The Journal of Neuroscience, April 1, 1999, 19(7):2834-2840

Lateralized Effects of Medial Prefrontal Cortex Lesions on Neuroendocrine and Autonomic Stress Responses in Rats
Ron M. Sullivan and Alain Gratton
Douglas Hospital Research Center, Department of Psychiatry, McGill University, Montréal, Québec Canada H4H 1R3

  ABSTRACT

TOP
ABSTRACT
INTRODUCTION
REFERENCES

The medial prefrontal cortex (mPFC) is highly activated by stress and modulates neuroendocrine and autonomic function. Dopaminergicinputs to mPFC facilitate coping ability and demonstrate considerablehemispheric functional lateralization. The present study investigatedthe potentially lateralized regulation of stress responses atthe level of mPFC output neurons, using ibotenic acid lesions.Neuroendocrine function was assessed by plasma corticosteroneincreases in response to acute or repeated 20 min restraint stress.The primary index of autonomic activation was gastric ulcer developmentduring a separate cold restraint stress. Restraint-induced defecationwas also monitored. Plasma corticosterone levels were markedlylower in response to repeated versus acute restraint stress. Inacutely restrained animals, right or bilateral, but not left mPFClesions, decreased prestress corticosterone levels, whereas inrepeatedly restrained rats, the same lesions significantly reducedthe peak stress-induced corticosterone response. Stress ulcerdevelopment (after a single cold restraint stress) was greatlyreduced by either right or bilateral mPFC lesions but was unaffectedby left lesions. Restraint-induced defecation was elevated inanimals with left mPFC lesions. Finally, a left-biased asymmetryin adrenal gland weights was observed across animals, which wasunaffected by mPFC lesions. The results suggest that mPFC outputneurons demonstrate an intrinsic right brain specialization inboth neuroendocrine and autonomic activation. Such findings maybe particularly relevant to clinical depression which is associatedwith both disturbances in stress regulatory systems and hemisphericimbalances in prefrontalfunction.

Key words: prefrontal cortex; asymmetry; ibotenic acid; stress ulcers; corticosterone; HPA axis; clinical depression; dopamine

  INTRODUCTION

TOP
ABSTRACT
INTRODUCTION
REFERENCES

The medial prefrontal cortex (mPFC) is an important region in mediating responses to stressful situations. This region isknown to modulate neuroendocrine function during stress by regulatingthe hypothalamic-pituitary-adrenal (HPA) axis (Feldman and Conforti,1985; Meaney and Aitken, 1985; McEwen et al., 1986; Diorio etal., 1993; Herman and Cullinan, 1997) and by acting as a sitefor glucocorticoids to exert negative feedback modulation of HPAactivity (Diorio et al., 1993). The mPFC also regulates a varietyof autonomic functions associated with stress in both rats (Henke,1984; Sullivan and Henke, 1986; Cechetto and Saper, 1990; Neafsey,1990; Frysztak and Neafsey, 1991, 1994; Henke et al., 1992) andhumans (Damasio et al., 1990; Damasio, 1994). The mPFC, in particularthe infralimbic and prelimbic cortices, can directly modulateneuroendocrine and autonomic function via projections to a numberof diencephalic, brainstem, and spinal control centers, and indirectlyvia projections to limbic areas that also regulate these regions(Terreberry and Neafsey, 1987; Hurley et al., 1991; Bacon andSmith, 1993).

The mesocortical dopamine (DA) projection originating in the ventral tegmental area provides an important modulatory inputto the mPFC. This projection is potently activated in times ofstress (Thierry et al., 1976; Deutch and Roth, 1990; Sullivanand Gratton, 1998) and plays a role in facilitating coping behaviorsand protecting against stress-related pathologies (Ray et al.,1988; Scatton et al., 1988; Carlson et al., 1993; Sullivan andSzechtman, 1995), presumably by dampening the activity of mPFCoutput neurons. Recent studies however, have revealed numerousleft/right hemispheric asymmetries in the mesocortical DA projectionin both basal conditions (Slopsema et al., 1982; Carlson et al.,1993; Sullivan and Szechtman, 1994; Sullivan et al., 1998) andin response to stress (Carlson et al., 1991, 1993, 1996; Sullivanand Szechtman, 1995; Sullivan and Gratton, 1998).

The purpose of the present study was therefore twofold. First, we sought to describe more precisely the role of the mPFC inregulating neuroendocrine and autonomic changes associated witheither acute or repeated stress by using ibotenic acid to destroythe intrinsic (including output) neurons of the mPFC. Second,we wanted to determine whether such manipulations of the leftand right mPFC reveal inherent functional asymmetries in the regulationof physiological stress responses, as their DAergic inputs havebeen shown todo.

As an index of neuroendocrine activation, we examined the elevation in plasma corticosterone (CORT) levels after either theacute or repeated exposure to a brief room temperature restraintstress. The primary index of autonomic responsivity was the formationof gastric ulcer pathology in response to a longer duration coldrestraint, a process known to be mediated by the vagus (Ray etal., 1987; Glavin et al., 1991).

  MATERIALS AND METHODS

Animals. Fifty-nine male Sprague Dawley rats (Charles River, St. Constance, Quebec) weighing 300-350 gm were used in the presentstudy. The animals were housed singly with food and water availablead libitum and were maintained on a 12 hr light/dark schedule(lights on at 8:00 A.M.). All procedures in the present studyconformed to the guidelines of the Canadian Council on AnimalCare.

Surgery and testing procedures. On the day of surgery, rats were pretreated with atropine sulfate (0.1 mg/kg, i.p.) and anesthetizedwith sodium pentobarbital (60 mg/kg, i.p.). Animals received eithersham (n = 17) or ibotenic acid lesions in the left, right, orbilateral mPFC (n = 14 per group). Two adjacent injection siteswere targeted in each hemisphere [anteroposterior (AP) +3.5, lateral(L) ±0.8 bregma, ventral (V) $-$ 4.7 from dura, and AP +2.5, L ±0.8,V $-$ 3.5 with skull horizontal as described in Paxinos and Watson,1982]. Solutions (5 µg/0.5 µl of ibotenate or saline vehicle)were injected via a 1 µl Hamilton microsyringe that was loweredstereotaxically into the brain. Each injection was performed overa 2 min period, with an additional 4 min allowed for diffusionaway from the tip of themicrosyringe.

Fifteen days after surgery, all rats were placed in Plexiglas large rodent restrainers for 20 min at room temperature, withblood samples (~50 µl) collected at 0, 20, and 80 min from thetip of the tail vein, to determine plasma CORT levels under prestress,peak, and recovery conditions, respectively. Rats were returnedto their home cages between the 20 and 80 min sampling periods.Samples were always collected between 10:00 A.M. and 2:00 P.M.Immediately after the 80 min sampling, rats underwent a 2.5 hrcold restraint stress (4°C) in the same restrainers, so that stressulcer formation could be assessed. This was the minimum durationof cold restraint required to reliably observe the developmentof gastric pathology in controlanimals.

As summarized in Table 1, rats in each lesion condition were randomly subdivided into acute and repeated restraint treatments,based on the 20 min room temperature restraint for plasma CORTassessment. The neuroendocrine data for the repeated groups thusrepresents the fifth exposure to the same (mild) stressor. Allrats in the study received a single, subsequent cold restraintstress on day 15.


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Table 1. Stress protocols of acute and repeated restraint treatments

As well, during the first four daily (20 min) restraint sessions in the repeated groups, the number of fecal boli were recordedduring the restraint sessions as a general index of autonomicreactivity. This measure was not recorded on the final test daywhen blood sampling was alsoconducted.

The inclusion of repeated (as well as acute) restraint groups allowed for the assessment of habituation of the plasma CORTstress response and for the possible dissociation of the mPFCregulation of an acute stress response versus one that incorporatesa learning/experiential component. This design also provided theopportunity to study whether repeated experience with a mild stressorwould be adaptive or maladaptive to the ability to cope with asubsequent more stressful situation (coldrestraint).

CORT assay. Plasma CORT levels were measured by radioimmunoassay as previously described by Krey et al. (1975) with a highlyspecific CORT antiserum (B3-163; Endocrine Sciences, Tarzana,CA) and ³H-CORT (101.0 µCi/mmol; New England Nuclear, Boston, MA) as tracer.The minimum level of detection with the assay is 1 ng/ml. Theantiserum cross-reacts slightly with desoxycorticosterone (~4%)but not with cortisol (<1%).

Stress ulcer assessment and histology. Immediately after cold restraint, animals were deeply anesthetized with chloral hydrate(400 mg/kg, i.p.). Stomachs were dissected out, cut along thegreater curvature, and washed in cold water. They were then examinedby an experimenter who was blind to the treatment conditions,with a dissecting microscope equipped with an ocular reticle andmeasured to the nearest 0.1 mm for the total length of mucosalhemorrhages (ulceration) in the glandular portion of the stomach.Adrenal glands were also dissected out at this time and weighedto the nearest 0.1 mg. Rats were perfused intracardially with0.9% saline and 10% formalin and brains removed for histologicalpurposes. Brains were later sectioned at 25 µm at $-$ 20°C and stainedwith thionin to determine the extent of ibotenate-induced cellloss in themPFC.

Statistical analysis. For the analysis of plasma corticosterone levels, acute and repeated restraint treatments were analyzedseparately, because these treatment differences were expectedto substantially affect this measure. For each treatment a two-factorANOVA was performed with factors of lesion (sham, left, right,bilateral) and sample (0, 20, and 80 min), with repeated measureson sample. The single dependent measure of gastric stress pathologywas examined with a two-factor (lesion × treatment) ANOVA. Theindex of defecation across days of restraint was analyzed witha two-factor (lesion × days) ANOVA with repeated measures on days.Finally, adrenal weights were analyzed with a three-factor (lesion× treatment × side) ANOVA with repeated measures on the withinsubjects factor of side (left or right adrenal). After significantmain effects or interactions, individual group comparisons wereperformed using Tukey's post hoc analysis. In addition, correlationalcomparisons were made between variables using Pearson's test ofcorrelation coefficients. All statistical tests were performedwith SPSS/PC+software.

  RESULTS

Histology

Figure 1, A and B, demonstrates the extent of ibotenate-induced cell loss in mPFC-lesioned animals. The minimum amount ofdamage in all lesioned animals included the infralimbic and prelimbiccortex as well as the rostral (pregenual) portion of the anteriorcingulate. Additional damage in a number of animals extended rostrallyto the ventromedial orbitofrontal cortex and posteriorly to morecaudal regions of (supragenual) cingulate, and in some cases dorsallyto the cortical surface in the region of the injection cannulatracts. In bilateral lesion groups, the extent of cortical lesionswas highly symmetrical in individual animals, and lesions in leftand right unilateral groups were indistinguishable in their extent.Unilateral lesions never infringed on the contralateral cortexand in no cases were subcortical structures affected. Finally,in no single group did variations in the total extent of lesionappear to be related to any of the stress measures obtained inthe study, suggesting that the most relevant cortical region orregions mediating the described effects on stress responses arethose within the area of minimal lesion-induced damage commonto all lesioned animals.

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Figure 1. Extent of ibotenate-induced cell loss in mPFC-lesioned rats. A depicts the typical degree of cell loss in infralimbic, prelimbic, and cingulate cortex, in this case in a right-lesioned animal. In B, black and shaded regions respectively represent the minimum and maximum extent of cell loss across animals. Numbers represent distance (in millimeters) anterior to bregma. See Results for additional detail.

Effects of lesions and treatments on plasma corticosterone profiles

Figure 2 depicts the plasma CORT levels across lesion and treatment conditions. Animals adapted markedly to the repeated restraintcondition; (initial analysis revealed a treatment effect of F_(1,51)= 83.46; p < 0.00005). The results of statistical analysis foracute and repeated treatments are detailed in the Figure 2 legend.Lesions of the mPFC reduced plasma CORT levels, such that withacute treatment, prestress levels were reduced by right or bilaterallesions, whereas in repeatedly restrained animals, stress-inducedincreases in CORT were suppressed by right or bilateral lesions.Left lesions did not significantly alter plasma CORT at any time.The large sample effects in each treatment condition reflect thetypically large CORT increases as a function of restraint.

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Figure 2. Effects of mPFC ibotenate lesions and treatments on mean (± SEM) plasma CORT levels in acutely (A) and repeatedly (B) restrained rats. The treatment difference in magnitude of CORT levels is reflected by the different scales of the two figures, because the CORT levels of repeated restraint groups were approximately half those of acute restraint animals at all time points, indicating a marked HPA adaptation to this stressor. Solid bars depict the 20 min period of restraint stress (room temperature). In acutely restrained animals, significant main effects were found for both lesion (F_(3,27) = 5.18; p = 0.006) and sample (F_(2,54) = 87.45; p < 0.0005), with no lesion × sample interaction. Although mPFC lesions tended to suppress CORT levels across samples, group differences were only significant at the prestress time point, because both right and bilateral groups were reduced relative to shams (Tukey's post hoc analysis; *p < 0.05). As with acute restraint, repeated restraint treatment revealed significant effects for lesion (F_(3,24) = 5.66; p = 0.004) and sample (F_(2,48) = 58.45; p < 0.0005) with no interaction. In this case, significant group differences were seen only in peak CORT levels, because both right and bilateral groups were significantly suppressed relative to shams (Tukey's post hoc analysis; *p < 0.05).

Lesion effects on cold restraint-induced gastric pathology

As demonstrated in Figure 3, mPFC lesions resulted in dramatic and highly asymmetrical reductions in stress ulcer formationresulting from the single exposure to cold restraint stress, regardlessof previous experience with acute or repeated mild stress (20min restraint at room temperature). Bilateral lesions greatlydecreased gastric stress pathology. Right lesions alone were ableto fully reproduce the effect of bilateral lesions, whereas leftmPFC lesions had no significant effect on this autonomically mediatedresponse to stress.

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Figure 3. Mean total ulcer length (± SEM) in mPFC-lesioned rats induced by a single 2.5 hr cold restraint session. A significant effect of mPFC lesion was observed (F_(3,58) = 8.98; p < 0.0005), with no significant effect of treatment and no lesion × treatment interaction. Regardless of previous experience with acute (A) or repeated (R) 20 min restraint stress, bilateral and right lesion groups each differed significantly from both the shams and left-lesioned animals (Tukey's post hoc analysis; *p < 0.05 in each case). Left-lesioned rats did not differ from shams, nor did right-lesioned rats differ from the bilateral lesion group. The inset reveals these pronounced lesion effect with treatments collapsed. S, L, R, and B refer to sham, left, right, and bilateral mPFC lesion groups, respectively.

Effects of cortical lesions on restraint-induced defecation

During once daily 20 min room temperature restraint sessions, left-lesioned animals were more frequently observed to struggleexcessively and to vocalize occasionally, unlike the other rats.The number of fecal boli was used as an index of emotional andautonomic reactivity, and as revealed in Figure 4, left-lesionedrats defecated more across days than other groups. Rats did notdemonstrate habituation on this measure across days of testing.

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Figure 4. Mean defecation in response to daily 20 min restraint sessions. A significant lesion effect was found on this measure (F_(3,24) = 6.82; p = 0.002), with no effect for days and no interaction for lesion × days. Rats with left mPFC lesions defecated to a greater extent than all other groups across days of testing.

Left/right asymmetry in mean adrenal weights

As depicted in Figure 5, left adrenal weights were significantly greater than right adrenal weights across animals. The mean(± SEM) weights for left and right adrenals across groups were29.6 (4.8) and 27.9 (4.5) mg, respectively. This measure was unaffectedby mPFC lesion or by restraint treatment conditions.

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Figure 5. Left/right asymmetry in mean adrenal weights. A significant main effect was observed for side (F_(1,51) = 7.56; p = 0.008), because the left adrenal was larger across animals. There were no significant effects for either lesion or treatment on this gross measure of neuroendocrine status, and no significant interactions were found. The A and R represent acute and repeated restraint treatment conditions, respectively.

Correlations between stress pathology and neuroendocrine measures

In general, stress ulcer pathology was positively correlated with plasma CORT levels, particularly in repeatedly stressedanimals. In these animals, the most notable correlation was betweenulcer pathology and peak CORT levels (r = 0.56; p = 0.002; n =28). The same relationship in acute animals failed to reach significance(r = 0.21,NS).

An additional measure of potential interest was individual adrenal gland asymmetry, computed as (L $-$ R)/(L + R), which wasfound to be related to stress measures in intact shams, but notin animals with mPFC manipulations. In acute shams, adrenal asymmetrywas significantly related to ulcer pathology (r = $-$ 0.72; p = 0.020;n = 10). In the repeated treatment shams this relationship waslost, however in this group, adrenal asymmetry was related toplasma corticosterone recovery levels (r = $-$ 0.82; p = 0.024; n=7).

  DISCUSSION

A principal finding of the present study was that mPFC lesions suppressed HPA activity in response to acute or repeated restraintstress. Either right or bilateral lesions reduced prestress plasmaCORT levels in acutely restrained animals, whereas the same lesionsin repeatedly restrained animals decreased the peak stress-inducedCORT response. Left mPFC lesions did not significantly affectplasma CORT levels. In response to cold restraint stress, mPFClesions caused a substantial and lateralized reduction in stressulcer pathology, as right brain lesions were both necessary andsufficient to inhibit ulcer formation, whereas left lesions werewithout effect. Restraint-induced defecation was increased byleft mPFC lesions alone, and adrenal gland weights exhibited aleft-biased asymmetry, regardless of lesion or treatmentconditions.

Before discussing the lateralized nature of mPFC lesion effects, it is necessary to comment generally on their direction.The inhibitory effects of ibotenate lesions on HPA function suggestthat mPFC output neurons normally stimulate the HPA axis. Thisis supported by the finding that electrical stimulation of thisregion increases plasma CORT levels (Feldman and Conforti, 1985).One study however, using bilateral thermal lesions of mPFC (includinganterior cingulate), reported no change in basal or peak plasmaCORT levels in response to 20 min restraint stress but an elevationin poststress recovery levels (Diorio et al., 1993). This apparentdiscrepancy may reflect lesion differences (additional fiber damagewith thermal lesions), placement differences (the present lesionsappear to involve a greater area of mPFC), and possibly additionalproceduraldifferences.

The lesion-induced suppression of stress ulcer formation is consistent with reports that electrolytic lesions or neuronalinhibition of mPFC and/or anterior cingulate decrease stress-inducedgastric pathology (Sullivan and Henke, 1986; Henke et al., 1992).Conversely, electrical stimulation or neuronal disinhibition ofthese regions increase gastric pathology (Henke, 1984; Sullivanand Szechtman, 1995).

The present decrease in plasma CORT levels as a function of repeated restraint parallels the habituation of HPA activationpreviously described after repeated experience with the same stressor(Hauger et al., 1990; Lachuer et al., 1994; Bhatnagar and Meaney,1995). Although less commonly noted, the present repeated restraintgroups also showed lower prestress CORT levels, perhaps indicatinga generalized adaptation to this particular procedure. Despitethe HPA adaptation to mild restraint, this experience was neitheradaptive nor maladaptive for subsequent stress ulcer formationafter cold restraint stress. Although HPA activation frequentlyhabituates with repeated same stress experience, stress responsesare often exaggerated after later exposure to a heterotypic stressor(Scribner et al., 1991; Aguilera, 1994; Bhatnagar and Meaney,1995). This pattern however, is not universal (Spencer and McEwen,1990; Aguilera, 1994) and depends on the stimulus properties (e.g.,intensity) of the stressors. The present results demonstrate thatdifferential experience with mild stress did not significantlyaffect the response to this heterotypic stressor and measure ofpathology.

An interesting association between these two stress measures emerged however, as plasma CORT levels and ulcer formation showedsignificant positive correlations in repeatedly but not acutelyrestrained animals. This suggests that whereas peak CORT responsesto acute stress may not predict susceptibility to stress pathology,failure to adapt to repeated mild stress may signify vulnerabilityto the pathological effects of more formidable stressors. Althoughcorticosteroids are known to be ulcerogenic (Borsch and Schmidt,1985), the above relationship does not imply causality, and interactionsbetween HPA mechanisms and autonomically mediated stress ulcerformation are highly complex (Glavin et al., 1991).

The pattern of lesion-induced suppression of HPA function differed between acute and repeated restraint treatments. Stress-inducedCORT elevations were reduced only in repeatedly restrained groups,suggesting a role for the mPFC in integrating experience withthe modulation of neuroendocrine function. Medial cortical modulationof stress ulcer development has also been shown to vary as a functionof experience, using a longer repeated stress protocol (Sullivanand Henke, 1986).

The present findings on HPA regulation suggest that an intact right mPFC is necessary for maximal stress-induced activation,particularly for previously experienced stressors. HPA functionin rats has been related to turning behavior (LaHoste et al.,1988), but not directly to cortical asymmetries. Human data however,suggest a normal right hemisphere dominance in the control ofcortisol secretion (Henry, 1997; Wittling, 1997). Furthermore,human studies have described the experience-dependent maturationof neural systems in corresponding frontal cortical regions, whichgenerate stress-regulating coping strategies and are lateralizedpredominantly to the right hemisphere (Schore 1996, 1997).

Indeed, the most notable aspect of the present findings concerns the extent of lateralized regulation of stress responsesat the level of the mPFC in the rat. Although cerebral lateralityin animals remains an underappreciated phenomenon, there are manysuch examples involving stress or emotionality-related processes,most commonly suggesting preferential roles for right brain mechanisms(Denenberg, 1981; Carlson et al., 1991, 1993, 1996; Davidson etal., 1992; Adamec and Morgan, 1994; Coleman-Mesches and McGaugh,1995; Sullivan and Szechtman, 1995; Sullivan and Gratton, 1998).

The presently reported cerebral asymmetry in the suppression of stress ulcer formation is consistent with findings of a similarstudy in rats using 6-hydroxydopamine lesions of the mPFC (Sullivanand Szechtman, 1995). The latter demonstrated that right but notleft lesions significantly increased cold restraint stress ulcers,most likely by disinhibiting the same mPFC neurons lesioned inthe present study. These studies suggest that although the rightmPFC may be necessary to mount a normal stress response, excessiveactivity of this region may be maladaptive. Prelimbic and infralimbicregions of mPFC are considered visceral motor regions and exertconsiderable influence over autonomic function (Cechetto and Saper,1990; Neafsey, 1990). Unfortunately, studies of lateralized autonomicregulation in rats are lacking. Human studies have described rightbrain dominance in autonomic activation in particular and emotionalexpression in general (Gainotti, 1983, 1987; Davidson, 1992; Wittling,1997; Meadows and Kaplan, 1994), and such processes have beenattributed importantly to the medial (orbital) prefrontal cortex(Damasio et al., 1990; Damasio, 1994; Schore, 1996, 1997).

The present measure of restraint-induced defecation was also asymmetrically affected by mPFC lesions, with left lesions increasingthis response. Considering defecation a physiological index ofemotional reactivity, this result profile conforms with earlierstudies examining the effects of large unilateral cortical lesionson various emotionality measures in rats (Denenberg, 1981; Denenbergand Yutzey, 1985). Although the right cortex was found to mediatesuch behaviors, the left cortex inhibited the emotional expressionof the right, as left lesions alone resulted in greater than controllevels on such measures. This pattern of results was not evidenton the present index of neuroendocrine function, although in bothtreatment conditions, there was a nonsignificant trend for leftlesions to produce the greatest stress-induced CORT elevationsas percent prestress levels (data not shown). The fact that leftlesions did not produce greater than control levels of gastricpathology may reflect the greater duration and intensity of coldrestraint stress. Data suggest that the left mPFC is specializedin generating coping strategies for mild or initial stress exposure,whereas right mPFC mechanisms predominate in situations of prolongedor uncontrollable stress (for detailed descriptions, see Carlsonet al., 1991, 1993; Sullivan and Szechtman, 1995; Sullivan andGratton, 1998). In the latter cases, interhemispheric influencesof the nature described above may be renderedineffective.

Finally, we report a left-biased asymmetry in adrenal gland weights, corroborating previous reports in both humans and rats(Freitas et al., 1978; Rubin and Phillips, 1991; Gerendai andHalasz, 1997). The present lesions and stress protocols did notdifferentially affect this gross measure. Variations in asymmetricaladrenal regulation have been related to various human pathologies,particularly depression (Otto et al., 1991; Wittling and Schweiger,1993; Szigethy et al., 1994). The left-biased adrenal asymmetrymay have an adaptive function, because in the present controlanimals, reversals of the normal adrenal asymmetry were correlatedwith increased ulcer pathology and elevated poststress CORT levels,possibly suggesting heightened vulnerability to stress. Theserelationships were less evident in animals with mPFCmanipulations.

Overall, the data suggest a preferential role for the right mPFC in activating physiological stress responses. Such specializationmay reflect perceptual processes and/or the integration of stress-relatedinputs with appropriate outputs for neuroendocrine and autonomicregulation. These data may have clinical relevance to major depressivedisorders, where heightened stress sensitivity and impaired copingability coexist with disturbances in both cerebral lateralityand stress-regulating systems (Barden et al., 1995). Studies haverevealed that either left frontal hypofunction or right frontalhyperfunction is associated with depressed states (Schaffer etal., 1983; Henriques and Davidson, 1991; George et al., 1996).Specifically, the left ventromedial prefrontal region exhibitsboth volumetric and metabolic reductions in unipolar and bipolardepressed patients (Drevets et al., 1997). Taken together withanimal findings, these studies emphasize the pathological potentialof imbalances within the mPFC, the functional distinctness ofthe left and right mPFC, and the need to study normal and abnormalasymmetries at thislevel.

  FOOTNOTES

Received Oct. 1, 1998; revised Jan. 19, 1999; accepted Jan. 24, 1999.

This research was made possible by grants from the Medical Research Council of Canada. A.G. is a holder of an FRSQ careerscientist award, and R.M.S. is a National Alliance for Researchon Schizophrenia and Depression Young Investigator. We thank DarleneFrancis for her assistance with the CORT assays and Dr. MichaelMeaney for his helpfulinsights.
Correspondence should be addressed to Dr. Ron Sullivan, Douglas Hospital Research Centre, 6875 LaSalle Boulevard, Verdun,Quebec, Canada H4H1R3.

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