Increase in Serotonin-1A Autoreceptors in the Midbrain of Suicide Victims with Major Depression---Postmortem Evidence for Decreased Serotonin Activity

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The Journal of Neuroscience, September 15, 1998, 18(18):7394-7401

Increase in Serotonin-1A Autoreceptors in the Midbrain of Suicide Victims with Major Depression $---$ Postmortem Evidence for Decreased Serotonin Activity
Craig A. Stockmeier¹^,², Laura A. Shapiro¹, Ginny E. Dilley¹, Tamara N. Kolli¹, Lee Friedman¹, and Grazyna Rajkowska³
¹ Program in Basic and Clinical Neuroscience, Department of Psychiatry, and ² Department of Neuroscience, Case Western Reserve University, Cleveland, Ohio 44106, and ³ Department of Psychiatry and Human Behavior, University of Mississippi Medical Center, Jackson, Mississippi 39216

  ABSTRACT

Top
Abstract
Introduction
Materials & Methods
Results
Discussion
References

It has been hypothesized that a deficit in serotonin may be a crucial determinant in the pathophysiology of major depression.Serotonin-1A receptors are located on serotonin cell bodies inthe midbrain dorsal raphe (DR) nucleus, and the activation ofthese receptors inhibits the firing of serotonin neurons and diminishesthe release of this neurotransmitter in the prefrontal cortex.Repeated treatment with some antidepressant medications desensitizesserotonin-1A receptors in the rat midbrain. The present studydetermined whether the binding of [³H]8-hydroxy-2-(di-n-propyl)aminotetralin (8-OH-DPAT), an agonistat serotonin-1A receptors, is altered in the midbrain of suicidevictims with major depression. Radiolabeling of the serotonin-1Areceptor in the DR varied significantly along the rostral-to-caudalextent of the human midbrain. The binding of [³H]8-OH-DPAT to serotonin-1A receptors was increased significantlyin the midbrain DR of suicide victims with major depression ascompared with psychiatrically normal control subjects. In suicidevictims with major depression, the increase in the binding of[³H]8-OH-DPAT to serotonin-1A receptors was detected in the entireDR and specifically localized to the dorsal and ventrolateralsubnuclei. Enhanced radioligand binding of an agonist to inhibitoryserotonin-1A autoreceptors in the human DR provides pharmacologicalevidence to support the hypothesis of diminished activity of serotoninneurons in suicide victims with major depression.

Key words: serotonin-1A receptors; dorsal raphe nucleus; major depression; suicide; postmortem brain

  INTRODUCTION

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Abstract
Introduction
Materials & Methods
Results
Discussion
References

Serotonin appears to play a key role in major depression and suicidality. Early evidence relating major depression to a decreasein serotonin neurotransmission comes from clinical observationsthat treatment with reserpine, a drug that depletes monoamineneurotransmitters, evoked clinical symptoms very similar to majordepression (Quetsch et al., 1959; Peterfy et al., 1976). Conversely,the symptoms of major depression are relieved by chronic treatmentwith medications that potentiate serotonergic activity by preventingeither the reuptake or the metabolism of serotonin (for review,see Montgomery, 1995).

Imaging studies suggest a role for the midbrain, a concentrated source of serotonin cell bodies, in the pathophysiology ofmajor depression. In a study that used ultrasound imaging, subjectswith major depression exhibited a significant trait-dependentdecrease in the reflection of ultrasound waves by the midbrainand pontine raphe as compared with normal controls, subjects withbipolar affective disorder, or subjects with schizophrenia (Beckeret al., 1995). Evidence for brainstem involvement in major depressionhas been demonstrated in a recent imaging study that showed thatpatients with major depression had a significant decrease in radioligandbinding to the serotonin transporter in the midbrain (Malisonet al., 1997).

Other research in completed suicide or suicide attempts provides evidence for reduced serotonin function in these individuals.In most, but not all, studies the content of serotonin or itsmetabolite, 5-hydroxyindoleacetic acid (5-HIAA), is decreasedin the brainstem of suicide victims (Shaw et al., 1967; Bourneet al., 1968; Pare et al., 1969; Lloyd et al., 1974; Beskow etal., 1976; Cochran et al., 1976; Korpi et al., 1986). Suicidalbehavior is associated with lower levels of 5-HIAA in the CSF,and there is evidence that suicide risk can be predicted by low5-HIAA in CSF after a suicide attempt (Nordstrom and Asberg, 1992).Finally, low serotonergic activity, as measured by the level of5-HIAA in the cerebrospinal fluid, is associated with plannedand more medically damaging suicide attempts in depressed patients(Mann et al., 1996).

Animal studies reveal that serotonin-1A receptors located on serotonin cell bodies in the midbrain influence the release ofserotonin in the prefrontal cortex. These receptors inhibit thefiring of serotonin neurons and diminish the release of this neurotransmitterin prefrontal cortex (Aghajanian et al., 1987). Serotonin-1A receptorsin the midbrain are desensitized by chronic treatment with antidepressantmedications such as monoamine oxidase inhibitors and selectiveserotonin reuptake inhibitors (SSRIs) (Blier and De Montigny,1994; Invernizzi et al., 1994). Therefore, changes in serotonin-1Areceptors in the human midbrain may alter the release of serotoninin prefrontal cortex and thereby play a significant role in majordepression.

The purpose of this study was to test the hypothesis that serotonin-1A receptors are increased in the dorsal raphe (DR) ofsuicide victims with major depression. The midbrain was sampledat several rostral-to-caudal levels, and quantitative receptorautoradiography was used to measure serotonin-1A receptors. Retrospectivepsychiatric assessments were used to select psychiatric subjectswith a current episode of major depression and comparison subjectsdetermined to be psychiatrically normal.

  MATERIALS AND METHODS

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Abstract
Introduction
Materials & Methods
Results
Discussion
References

Subjects. Brain tissue was obtained at autopsies performed at the Cuyahoga County Coroner's Office, Cleveland, OH. The studywas performed in compliance with policies of an institutionalreview board, and written consent was obtained from the next-of-kin.Midbrains were collected from 10 suicide victims and 10 age-matched(± 5 years) comparison subjects dying of natural or accidentalcauses. The causes of death were certified by the County Coronerand are listed in Table 1. Both tissues and the resultant autoradiogramsfrom the matched pairs of subjects were coded and then processedand analyzed in parallel.


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Table 1. Characteristics of subjects

The toxicology laboratory of the County Coroner's Office examined blood and urine samples from the subjects. Qualitative andquantitative assays were used to detect the compounds and theirmetabolites, as previously described (Stockmeier et al., 1997).The results of the toxicology testing are listed in Table 1.

Retrospective psychiatric diagnoses. Retrospective psychiatric assessments were used as previously described to identify controlsubjects without a mental illness and suicide victims with a currentdiagnosis of major depression (Stockmeier et al., 1997). Kellyand Mann (1996) recently have validated the use of psychologicalautopsy by demonstrating good agreement between informant-basedretrospective psychological assessments of deceased subjects andchart diagnoses generated by clinicians treating the same subjectsbefore death. In the current study, ~3 months after death, a trainedinterviewer administered a structured interview with a knowledgeableinformant for all 20 of the subjects to collect information fordetermining the presence or absence of psychiatric disorders.Knowledgeable informants either lived with or had frequent weeklycontact with the subjects before death. Data on lifetime and currentmental illness were gathered with a modified Schedule for AffectiveDisorders and Schizophrenia: Lifetime version (SADS-L; Spitzerand Endicott, 1978). Diagnoses for Axis I disorders were assessedindependently by a clinical psychologist and psychiatrist, andconsensus diagnosis was reached in conference, using all availableinformation from the knowledgeable informants, the coroner's office,and previous hospitalizations and doctors' records. The finaldiagnosis was compatible with the Diagnostic and Statistic Manualof Mental Disorders-Revised (DSM-III-R; American Psychiatric Association,1987). The psychiatric diagnoses are summarized in Table 1.

The suicide victims met diagnostic criteria for a current history of major depression during the last month of life. One suicidevictim with major depression also had a current comorbid diagnosisof dysthymia. There was no current psychoactive substance disorder(abuse or dependence) in any of the subjects. Three suicide victimspreviously met diagnostic criteria for alcohol abuse at 2, 4,and 24 years before death. Another suicide victim met diagnosticcriteria for alcohol dependence at 15 years before death. Twopsychiatrically normal control subjects met criteria for alcoholabuse at 7 and >2 years before death.

Tissues and immunohistochemistry. The midbrains were isolated from the brainstem by making a transverse cut along a line fromthe rostral border of the superior colliculus to the exit pointof the oculomotor nerve. A second cut at the level of the isthmuswas made along a line from the caudal extent of the inferior colliculus(at the exit of the trochlear nerve) through the pontine tegmentum.Tissues were frozen in isopentane cooled by solid CO₂ and storedat $-$ 80°C until the assays were performed. Tissue samples werecoded to conceal the diagnostic group of the subjects.

The midbrain blocks were mounted on pedestals with Tissue-Tek (Miles, Elkhart, IN), and frozen sections were cut at $-$ 15°Cwith a microtome (IEC, Needham Heights, MA). Sections for serotonin-1Areceptor autoradiography were cut at 20 µm thickness, and serialsections for tryptophan hydroxylase (TrpOH) immunohistochemistrywere cut at 30 µm thickness. Sections were thaw-mounted onto coldmicroscope slides coated with gelatin/chrom-alum, dried undera stream of room-temperature air, and refrozen at $-$ 80°C. At 0.5mm intervals along the block of tissue, sections were taken forboth immunohistochemistry and receptor autoradiography. Slidesfor TrpOH immunohistochemistry were used to identify anatomicallycomparable rostral-caudal levels for analysis and to localizethe subnuclei of the DR, as described by Baker et al. (1990, 1991).From a rostral-to-caudal direction, corresponding levels betweensubjects were identified by using the following description ofanatomical landmarks. At level A, the oculomotor nucleus and thedorsal and ventral subnuclei of the DR (DRd, DRv) were present.At level B, the oculomotor nucleus was absent, and the trochlearnucleus appeared. The interfascicular subnucleus (DRif) was presentat level B. Level C revealed a prominent trochlear nucleus thatwas traversed by the trochlear nerve and its root. The ventrolateralsubnucleus (DRvl) of the DR appeared and extended laterally atthis level. The trochlear nucleus and DRvl were present at levelD. At level E, the trochlear nucleus was absent, and the DRvlwas less prominent and located more medially than at level C.Level F included the compact interfascicular nucleus, the decussatingfibers of the superior cerebellar peduncles, DRd and DRv, andthe most rostral traces of the LC. In level G, the median raphenucleus was present and penetrated by the decussating fibers ofthe superior cerebellar peduncles. Level H was similar to levelG, except that the median raphe nucleus was more or less penetratedby the decussating fibers of the superior cerebellar peduncles.Level H included the caudal subnucleus of the DR (DRc) that extendedboth medially and laterally in the ventral direction. Level Iincluded the LC, median raphe nucleus, fourth ventricle, mediallongitudinal fasciculus, and the DRc. A randomly selected midbrainwas used as a standard to which the rostral-to-caudal levels ofthe other midbrains were compared and with which they were setin register. Although the midbrain consistently was blocked anddissected from each subject, there were slight variations in therostral-to-caudal appearance and disappearance of the varioussubnuclei of the DR in the 20 subjects. Hence, the most rostraland most caudal levels of the midbrain are not presented in Figure2.

Receptor autoradiography. Radioligand binding to serotonin-1A receptors was determined autoradiographically, as describedby Stockmeier et al. (1996), using the serotonin-1A receptor agonist[³H]8-hydroxy-2-(di-n-propyl)aminotetralin (8-OH-DPAT). After a30 min preincubation at room temperature in buffer (pH 7.7 at24°C) containing 170 mM Tris-HCl, 4 mM CaCl₂, and 0.01% ascorbicacid, three sections were incubated in fresh buffer for 1 hr at24°C with [³H]8-OH-DPAT (2 nM, 154.3 Ci/mmol; New England Nuclear, Boston,MA). Nonspecific binding was measured in duplicate serial sectionscoincubated with 10 µM serotonin (serotonin creatinine sulfatecomplex; Sigma, St. Louis, MO). Citalopram-hydrobromide (1 µM;Lundbeck, Copenhagen, Denmark) was included in the incubationwith [³H]8-OH-DPAT because there is evidence in rat striatum as wellas bovine DR that [³H]8-OH-DPAT binds to the serotonin transporter in addition tothe serotonin-1A receptor (Alexander and Wood, 1988; Sprouse etal., 1993).

After the incubation the sections were washed twice at 4°C for 5 min each in the same (nonradioactive) buffer (pH 7.7 at 4°C).Sections were dipped in ice-cold water, air-dried, and storedfor 24-48 hr at 4°C in sealed slide boxes with Drierite capsules.The sections and tritiated plastic standards (American RadiolabeledChemicals, St. Louis, MO) that had been calibrated to brain mashwere apposed to Hyperfilm-³H (Amersham, Arlington Heights, IL) in x-ray cassettes for 1 week.Films were processed with Kodak D-19 developer and fixed withKodak Rapid Fix (Eastman Kodak, Rochester, NY).

Autoradiographic images of radioligand binding in the DR were digitized and quantitated with the Microcomputer ControlledImaging Device (MCID; Imaging Research, St. Catharine's, Ontario,Canada). The subnuclei of the DR were identified by the cellularcriteria of Baker et al. (1990, 1991) with a projection microscopein slides immunohistochemically stained for TrpOH. The bordersof the subnuclei were drawn on paper, and digital templates ofthe borders were constructed from digitized images of the TrpOHimmunohistochemistry. The digital templates of the borders weresuperimposed by MCID on autoradiographic images of serotonin-1Areceptor binding. For each section, serotonin-1A receptors weremeasured in the entire midline DRif and the left half of eachof the other subnuclei as well as in a composite image of thesesubnuclei. Total binding of [³H]8-OH-DPAT was quantified and regarded as specific binding, inasmuchas nonspecific binding was nearly indistinguishable from filmbackground.

Data analysis and statistics. Ten matched pairs of controls and suicide victims were used for the group-by-level analysisof [³H]8-OH-DPAT binding to serotonin-1A receptors. There were fivedependent variables, each measured at three to five levels (seeFig. 2; whole, levels C-G; ventrolateral, levels E-G; dorsal,levels D-G; interfascicular, levels C-G; and ventral, levels D-G),for a total of 21 measurement sites.

Because the specimens were processed as age-matched pairs of controls and suicide victims, a paired ANOVA analysis was performed,with two within-subjects (repeated measures) factors, i.e., groupand level. Statistically significant group-by-level interactionswere followed up with paired Student's t tests at each level todetermine the rostral-caudal location of any group differences.The ages and postmortem intervals (time between death and freezingof the tissue) of the two groups of subjects (n = 10 per group)were compared with paired Student's t tests. An ANCOVA also wasperformed, with age and postmortem interval as covariates. Theresults of the ANCOVA were not substantially different from theANOVA with repeated measures (data not shown).

  RESULTS

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Abstract
Introduction
Materials & Methods
Results
Discussion
References

The binding of [³H]8-OH-DPAT to serotonin-1A receptors was measured in 10 pairs of psychiatrically normal control subjectsand age-matched suicide victims with major depression. Characteristicsof the subjects are presented in Table 1. The average age ofthe control subjects was 52 ± 5 years (mean ± SEM), and that ofthe suicide victims was 50 ± 6 years. The average postmortem intervalof the control subjects was 17 ± 2 hr and of the suicide victimswas 18 ± 2 hr. There was no significant difference between subjectgroups for either age or postmortem interval.

The specific binding of [³H]8-OH-DPAT is highly localized to the DR in the human midbrain. For orientation, a schematic drawingof the midbrain DR and its subnuclei is presented in Figure 1.As observed previously (Stockmeier et al., 1996), serotonin-1Areceptors are located differentially along the midbrain DR. Thereis a strong main effect of rostral-to-caudal level for the entireDR as well as for each subnucleus (Table 2; Fig. 2). For theentire DR the autoradiographic density of serotonin-1A receptorsat the middle levels of the midbrain (levels D and E) is nearlytwice that detected more rostrally or caudally. When subnucleiof the DR are examined, the greatest amount of [³H]8-OH-DPAT binding occurs in the DRvl and DRv subnuclei at levelsE and F, where serotonin-1A receptors are observed at ~600 fmol/mgof protein. The density of serotonin-1A receptors in the DRd andDRif is approximately one-half that of the DRvl and DRv.

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Figure 1. Schematic drawings of the human dorsal raphe nucleus (DR). The drawing in A represents a transverse section of the midbrain at the level of the inferior colliculus. The boxed area depicts the location of the DR in the ventral region of the central gray matter. B is an enlargement of the boxed area in A and demonstrates the cerebral aqueduct (Aq), the nucleus of the trochlear nerve (cranial nerve 4), and the dorsal (DRd), ventral (DRv), ventrolateral (DRvl), and interfascicular (DRif) subnuclei of the DR.


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Table 2. Analysis of effects of rostral-caudal level and diagnostic group on serotonin-1A receptors in the dorsal raphe of 10 pairs of suicide victims with major depression and normal control subjects

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Figure 2. The distribution of [³H]8-hydroxy-2-(di-n-propyl)aminotetralin binding to serotonin-1A receptors in the entire midbrain dorsal raphe (DR) or various subnuclei along rostral-to-caudal levels of the midbrain from 10 pairs of suicide victims with major depression and age-matched psychiatrically normal control subjects. The abscissa represents 0.5 mm levels through the midbrain, with rostral levels located to the left. The ordinate represents [³H]8-OH-DPAT binding (fmol/mg protein) to serotonin-1A receptors. See Materials and Methods for a description of the criteria used for delineating the rostral-to-caudal levels. Serotonin-1A receptors were enhanced significantly in depressed suicide victims (statistically significant main effect of subject group) in the entire DR (A; p < 0.021) and in ventrolateral (B; p < 0.004) and dorsal (C; p < 0.004) subnuclei, but not in interfascicular (D) or ventral (E) subnuclei, as compared with psychiatrically normal control subjects.

There was a statistically significant main effect of subject group for the entire DR as well as for DRd and DRvl subnuclei(Table 2; Fig. 2) (ANOVA for repeated measures). Within the entireDR, the DRd, and the DRvl the significant increase in serotonin-1Areceptors in depressed suicides ranged from 5 to 30%, from 11to 34%, and from 11 to 13%, respectively, depending on the rostral-to-caudallevel. There was a trend toward a significant increase in serotonin-1Areceptors in the DRv, but it did not reach statistical significance.The main effect of subject group is demonstrated in colorizeddigital autoradiograms from four representative levels of a depressedsuicide victim and the matched control (Fig. 3). The pattern ofresults of increased serotonin-1A receptors in depressed suicideswas essentially the same when an ANCOVA was performed with ageand postmortem interval as covariates (data not shown).

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Figure 3. [³H]8-hydroxy-2-(di-n-propyl)aminotetralin binding to serotonin-1A receptors in the midbrain dorsal raphe (DR) from a representative control subject that was psychiatrically normal (left) and an age-matched suicide victim with major depression (right). The control subject was the 27-yr-old male, and the suicide victim was the 30-yr-old male (see Table 1). The digitized autoradiograms of the DR are shown at four rostral-to-caudal levels of the midbrain, with the upper images located more rostrally. Note the enhanced radioligand binding to serotonin-1A receptors in the depressed suicide victim, as evidenced by greater numbers of orange and red pixels in the images in the right column. The distance across the widest portion of the DR is ~5 mm.

The overall pattern of the rostral-to-caudal distribution of serotonin-1A receptors within the midbrain DR was studied inboth subject groups by examining level-by-group interactions.For the entire DR as well as for the subnuclei, including theDRd, DRv, and DRvl, the overall pattern of the rostral-to-caudaldistribution of serotonin-1A receptors along the midbrain (i.e.,the shape of the curves) did not differ between controls and suicidevictims (Table 2). The interaction of level-by-group was statisticallysignificant only for the DRif, although follow-up Student's ttests did not reveal a statistically significant group effectat any single level of the DRif (Table 2).

  DISCUSSION

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Abstract
Introduction
Materials & Methods
Results
Discussion
References

The binding of [³H]8-OH-DPAT to serotonin-1A receptors was increased significantly in the midbrain DR of suicide victims withmajor depression as compared with psychiatrically normal controlsubjects. The increase in serotonin-1A receptors was detectedwithin the entire cross section of the midbrain DR and specificallylocalized to the DRd and DRvl subnuclei. Our evidence in thesesubjects indicates that major depression, suicide, or the combinationof these two factors is related to a significant and consistentincrease in serotonin-1A receptors at several levels along themidbrain DR. It remains to be determined whether the increasein [³H]8-OH-DPAT binding in the midbrain DR of depressed suicides isan increase in receptor number (B_max) or affinity (K_D). The designof the current autoradiography study did not permit a determinationof binding maxima.

Several groups have examined serotonin-1A receptors located in prefrontal cortex in suicide victims; however, a clear picturehas not emerged. Arango et al. (1995) reported increases in radioligandbinding to serotonin-1A receptors in ventrolateral prefrontalcortex of suicide victims. Other studies in suicide victims whowere characterized psychiatrically report no change in serotonin-1Areceptors in other regions of prefrontal cortex (Arranz et al.,1994; Lowther et al., 1997; Stockmeier et al., 1997). In contrastto presynaptic serotonin-1A receptors in the DR, serotonin-1Areceptors in prefrontal cortex are located postsynaptically, andtheir involvement in depression and suicide awaits further clarification.

Potential limitations of the current study include the use of retrospective informant-based data for psychiatric determinations,comorbid psychoactive substance use disorders, and the potentialeffects of medications. In a recent validation of the psychologicalautopsy technique, Kelly and Mann (1996) reported a 91% agreementbetween DSM-III-R diagnoses made antemortem by treating cliniciansand informant-based diagnoses made postmortem. The current studyis one of few postmortem studies in suicide in which retrospectivelycollected psychiatric information is presented for both the experimentaland control groups. In our selection of subjects we attemptedto rule out any contribution of a psychoactive substance use disordersuch as alcohol dependence or abuse to serotonin-1A receptorsin the midbrain. Only one suicide victim ever met criteria foralcohol dependence (15 years before death). Furthermore, of thetwo control subjects and three suicides that at one time met criteriafor alcohol abuse, between 2 and 24 years had elapsed betweenthe end of the alcohol abuse and the deaths. Two suicide victimswere exposed to benzodiazepine medications at or about the timeof their deaths; however, chronic treatment with diazepam doesnot alter the function of the serotonin-1A autoreceptor in theDR (Wilson and Gallager, 1988).

Alterations in serotonin-1A receptors in depressed suicide victims may be related to exposure to antidepressant medications.Two of the suicide victims were taking an antidepressant medicationin the last month of life, and two others had prescriptions forantidepressant medications in the year preceding their deaths.There was no evidence in blood or urine of the recent presenceof these medications or their metabolites. Because not all ofthe subjects had recent exposure to antidepressant medications,it appears that the increase in serotonin-1A receptors is relatedto the depression and/or suicide. Furthermore, chronic treatmentof rats with SSRIs, monoamine oxidase inhibitors, or novel anxiolyticswith antidepressant qualities either decreases or has no effecton [³H]8-OH-DPAT binding to serotonin-1A receptors in midbrain (Welneret al., 1989; Gobbi et al., 1991; Hensler et al., 1991; Fanelliet al., 1992; Burnet et al., 1994; Le Poul et al., 1995).

The role that serotonin-1A receptors in the DR plays in depression and suicide may be related to the location of these receptorson serotonin neurons and the ability of these receptors to regulatethe electrical activity of serotonin neurons. The serotonin-1Areceptor protein is synthesized by serotonin neurons in the DR,and immunohistochemical evidence reveals that nearly all of thesereceptors are located on the perikarya and dendrites of serotoninneurons (Sotelo et al., 1990; Miquel et al., 1992). The serotonin-1Areceptor has been classified functionally as an inhibitory autoreceptor,because the firing rate of serotonin neurons in the DR is inhibitedby the direct application of 8-OH-DPAT, a serotonin-1A receptoragonist, into the DR (Sprouse and Aghajanian, 1986). Thus, theobserved increase in presumably inhibitory serotonin-1A receptorsin the DR of suicide victims with major depression may providepharmacological evidence for diminished activity of serotoninneurons in these subjects.

In the study of the human DR, it is important to identify comparable rostral-caudal levels for biological comparisons betweengroups of subjects. Serotonin-containing neurons within the humanDR have been grouped into five subnuclei on the basis of neuronalmorphology and density (Baker et al., 1990, 1991), and the locationsand boundaries of these subnuclei vary along the extent of themidbrain. In the current study there was a strong influence onradioligand binding of the rostral-caudal level for the entireDR as well as for each subnucleus. Consequently, sections werecollected at 0.5 mm intervals, landmarks were used to identifythe levels, and anatomically equivalent rostral-caudal levelswere examined in the subject groups.

Functional abnormalities detected in prefrontal cortex in depression may be related to abnormalities in specific subregionsof the brainstem DR. A coarse topographic organization has beendescribed for the primate DR as related to its target areas inthe cerebral cortex. Wilson and Molliver (1991) have observedthat clusters of neurons in the DR project to different corticalassociation areas, and they propose that clusters of neurons maybe related to different higher functions. For example, tract-tracingstudies in nonhuman primates reveal that many of the DR neuronsprojecting to the dorsolateral prefrontal cortex originate inthe midbrain DR. In a recent functional imaging study of subjectswith major depression who responded to SSRIs, an acute depletionof the serotonin precursor tryptophan resulted in a relapse indepressive symptoms and a decrease in brain metabolism in dorsolateralprefrontal cortex (Bremner et al., 1997). It is interesting tospeculate that altered function of serotonin-1A autoreceptorson serotonin cell bodies in the midbrain DR in major depressionmay be related to brain metabolism affected by tryptophan depletionin dorsolateral prefrontal cortex in major depression. Postsynapticserotonin-1A receptors and serotonergic fibers from the midbrainDR are highly concentrated in outer layers of prefrontal cortex(Smiley and Goldman-Rakic, 1996; Stockmeier et al., 1997). Itremains to be determined whether postsynaptic serotonin-1A receptorsin dorsolateral prefrontal cortex are altered in the same suicidevictims with major depression that demonstrate increased serotonin-1Aautoreceptors in the midbrain DR.

Serotonin-1A receptors in the midbrain DR may be critical to the therapeutic effect of some antidepressant treatments, asrevealed by electrophysiological experiments. Serotonin-1A receptorsin the DR are desensitized by the repeated treatment of experimentalanimals with a monoamine oxidase inhibitor or SSRI (Blier et al.,1986; Chaput et al., 1988), and that desensitization is coupledwith a facilitation of serotonin output in the frontal cortex(Invernizzi et al., 1994). Thus, the therapeutic action of someantidepressant treatments in humans may involve the facilitationof serotonin neurotransmission in prefrontal cortex in responseto desensitization of inhibitory serotonin-1A autoreceptors inthe midbrain DR (Blier and De Montigny, 1994). In this study theobservation of increased serotonin-1A receptors in the midbrainDR of suicide victims with major depression is consistent withthe hypothesis that the therapeutic effect of antidepressant medicationsmay involve at least physiological desensitization (if not downregulation)of these receptors on serotonin neurons.

It has been suggested that serotonin-1A autoreceptors in the midbrain play a role in hastening the antidepressant effect ofSSRIs (Artigas et al., 1996). Two open-label studies reportedthat pindolol, an antagonist at $beta$ -adrenergic and serotonin-1Areceptors, induced a rapid improvement in depressive symptomsin patients treated with an SSRI or monoamine oxidase inhibitor(Artigas et al., 1994; Blier and Bergeron, 1995). Artigas et al.(1996) suggest that the 2 week delay in the onset of the therapeuticbenefit of antidepressant medication may be attributable to theability of an SSRI to increase the extracellular concentrationof serotonin in the midbrain DR, thereby activating inhibitorysomatodendritic serotonin-1A autoreceptors. As a result of a diminishedfiring of serotonin neurons, the extracellular concentration ofserotonin in the cerebral cortex would be diminished early inthe course of SSRI therapy. Cotreatment with pindolol, it washypothesized, would restore the firing of serotonin neurons byblocking the inhibitory somatodendritic serotonin-1A autoreceptorsand increasing extracellular serotonin concentrations in the forebrain,thereby decreasing the latency of the antidepressant response(Blier and Bergeron, 1997). Most, but not all, double-blind placebo-controlledstudies of pindolol plus an SSRI support the hypothesis that pindololaccelerates the antidepressant response (Berman et al., 1997;Perez et al., 1997; Tome et al., 1997; Zanardi et al., 1997).

Future studies in subjects with major depression not dying by suicide and in suicide victims not meeting criteria for majordepression will help to identify whether increased serotonin-1Areceptors in the midbrain DR are associated with suicide per se,major depression, or an interaction between major depression andsuicide. The postmortem evidence reported here provides a clearimpetus for the continued development of radioligands for theserotonin-1A receptor to be used in positron emission tomographystudies of the DR in patients with major depression and/or suicidalbehavior (Farde et al., 1997).

  FOOTNOTES

Received May 14, 1998; revised June 22, 1998; accepted June 29, 1998.

This work was supported by grants from the National Institute of Mental Health (MH45488) and The American Foundation for SuicidePrevention. We gratefully acknowledge the work of Herbert Y. Meltzer,M.D., and James C. Overholser, Ph.D., in the retrospective psychiatricdiagnoses. The excellent assistance of the Cuyahoga County Coroner'sOffice, Cleveland, OH, is greatly appreciated. Helpful conversationswith Gregory Ordway, Ph.D., and the technical assistance of JinrongWei are gratefully noted.
Correspondence should be addressed to Craig Stockmeier, Ph.D., Department of Psychiatry, Hanna Pavilion B-68, University Hospitalsof Cleveland, 11100 Euclid Avenue, Cleveland, OH 44106-5078.

  REFERENCES

Top
Abstract
Introduction
Materials & Methods
Results
Discussion
References

Aghajanian GK, Sprouse JS, Rasmussen K (1987) Physiology of the midbrain 5-HT system. In: Psychopharmacology: the third generation of progress (Meltzer HY, ed), pp 141-148. New York: Raven.
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