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Published Online: February 1998

The Use of Rapid-Rate Transcranial Magnetic Stimulation (rTMS) in Refractory Depressed Patients

Publication: The Journal of Neuropsychiatry and Clinical Neurosciences

Abstract

Rapid-rate transcranial magnetic stimulation (rTMS) allows for the noninvasive examination of the cerebral cortex. Recent studies have begun to investigate whether rTMS may be therapeutic for the treatment of depression. In the present study, the authors report on the safety and efficacy of rTMS in treating 50 patients with refractory depression. Overall, there were 21 responders (42%). Interestingly, 56% of the young patients responded, but only 23% of the elderly patients responded to rTMS. Overall, rTMS was well tolerated in all patients. Specifically, no patient developed a new onset of seizures during rTMS. The authors discuss the extant literature on rTMS for the treatment of depression along with future areas of research.
Rapid-rate transcranial magnetic stimulation (rTMS) allows for the noninvasive examination of the cerebral cortex.1 rTMS stimulates the cerebral cortex with magnetic fields resulting from current passing through a wire coil on the scalp. Transcranial magnetic stimulation has been used to investigate brain functions such as attention, memory, movement, speech, and vision. In addition, rTMS is beginning to be used to investigate the pathophysiology of Parkinson's disease.1
Recent works have also suggested that rTMS may be used for exploring the functional neuroanatomy of emotions. Specifically, two TMS studies reported that healthy volunteers who received left prefrontal stimulation reported an increase in self-rated sadness; in contrast, right prefrontal stimulation caused an increase in happiness.2,3
On the basis of these results, along with observations in functional and structural imaging studies that frontal lobe abnormalities exist in some patients with depression, rTMS studies have begun to investigate whether rTMS may be therapeutic for the treatment of depression.4 The initial reports using TMS for the treatment of depression were “open label” and stimulated the center of the head. The results of these early studies were promising.57 Subsequently, George et al.8 at the National Institute of Mental Health employed rTMS over the prefrontal cortex in 6 treatment-refractory depressed patients and observed improvement in 2 of their patients. The largest rTMS study of depression to date was done by Pascual-Leone et al.9 They used a crossover placebo-controlled study design. The authors reported that left prefrontal rTMS was effective in treating 11 of 17 young (less than 60 years of age) depressed patients. All of the patients were either medication resistant or psychotic. Interestingly, left prefrontal rTMS was found to be more effective than rTMS using right-sided or more posterior anatomic stimulation sites. None of the patients in this study experienced any significant side effects from rTMS.
More recently, George et al. have completed a double-blind, randomized crossover study in 12 depressed outpatients.10 Patients in this study received placebo or left prefrontal rTMS. The authors have reported a statistically significant improvement in mood for the rTMS over the placebo group.
On the basis of these studies, we decided to conduct an open, prospective trial that examined the use of left prefrontal rTMS in the treatment of patients with refractory depression. The goals of this study were:
1.
To examine whether rTMS is effective in the treatment of a larger sample of treatment-resistant, young (less than 65 years of age) depressed patients.
2.
To examine the safety and efficacy of rTMS in treating a group of depressed elderly patients and compare their response rates with those observed in the young depressed patients who received rTMS. To date, rTMS has not been examined for the treatment of elderly depressed patients. As a result, the question of whether rTMS can be safely and effectively used in the depressed elderly remains unanswered.
3.
To examine some clinical characteristics that may be predictive of a therapeutic response from rTMS.
4.
To describe any side effects from rTMS that may develop during the course of this study.

METHODS

Subjects

Between January 1996 and March 1997, 56 patients received a course of rTMS at Wesley Woods Geriatric Hospital/Emory University Medical Center. All 56 patients and their families gave informed consent to a protocol approved by the Human Investigations Committee of the Emory University School of Medicine and by the research committees of both hospitals. All 56 patients were referred to the Mood Disorders Clinic at Wesley Woods Geriatric Hospital. Forty-four of these patients had been referred for electroconvulsive therapy (ECT) and chose to receive rTMS prior to ECT. Fifty-three of the patients (94%) had received at least a 6-week trial of an antidepressant at a therapeutic dose (Table 1). Seventeen patients had a prior history of receiving ECT. There were 31 women and 25 men among the 56 patients who received rTMS. The patients ranged in age from 22 to 89, with a mean age of 60 years.
All patients met DSM-IV criteria for a major depressive episode (53 unipolar, 3 bipolar). All patients were rated at least moderately ill on the Clinical Global Impression Scale and had a pretreatment score on the 21-item Hamilton Rating Scale for Depression (Ham-D) of greater than 20 (mean score of 34). In addition, 4 patients had a DSM-IV diagnosis of dementia. All diagnoses were made by a physician (G.S.F.) using a DSM-IV checklist during a structured clinical interview. The Folstein Mini-Mental State Examination (MMSE) was administered to 54 of the 56 patients before they received rTMS administered by a member of the treatment team (J.A.-L.). Two patients were not able to perform the mental status examination because of the severity of their illness.
In general, patients were tapered off their psychotropic medications prior to beginning their course of rTMS. A few patients (n=6) were unable to be tapered off their medications because of the severity of their illness. In no case was a patient started on a new psychotropic medication during rTMS treatments. The patients who remained on psychotropic medications had been on these medications for several months. As a result, any change in these patients' clinical status during rTMS was not felt to be attributable to the concomitant use of the psychotropic medications.
Many (n=21) of the patients had a history of one or more of the following medical illnesses: hypertension and/or coronary artery disease (n=21), congestive heart failure (n=2), history of transient ischemic attacks (n=3), diabetes mellitus (n=6), or cerebral vascular accident (n=1). Patients with a history of a recent myocardial infarction, cardiac pacemaker, intracranial metallic objects, or an increased intracranial pressure were excluded from the study.
The patients were classified as responders according to the criteria of Sackeim et al.11 They had to show a 60% reduction from their pretreatment Ham-D score, as well as a posttreatment Ham-D score of 16 points or less. In addition, patients had to be rated as moderately to markedly improved on a 7-point Clinical Global Impression Scale. These ratings were completed by the patient's clinical treatment team along with the physician on the rTMS service (G.S.F.). All ratings were obtained prior to beginning rTMS and within 48 hours after the fifth treatment.

rTMS Methods

All treatments were administered in the ECT laboratory, once daily for 5 consecutive weekdays. If there was no clinical response after 5 treatments, rTMS was stopped. Patients lay supine with the head elevated on a pillow. Continuous cardiac monitoring was performed, and blood pressure was taken every 60 seconds during stimulation.
High-speed rTMS was performed with a custom device, using a damped cosine pulse and a prototype iron-core magnetic coil. The latter induces electric fields similar in distribution to those from a Cadwell water-cooled figure-eight coil but is much smaller, quieter, and more efficient, requiring no special cooling. This coil also has an open port in the center for precisely marking and reproducing position on the head.
Relaxed motor threshold and the location of the right-hand motor area were identified over the left hemisphere as previously described.12 During stimulation at a rate of 1.0 Hz, the magnetic coil was moved across the left central region and the stimulator output was gradually increased to locate the point of lowest-intensity activation, followed by the magnetic threshold at that site. This position was then labeled with a permanent marker. Determining motor threshold required only 5 to 10 minutes at the first treatment session, and less time on subsequent days because the location had been marked. The site of rTMS treatment was then measured 5 cm anteriorly from the hand motor area on a sagittal line.
For each rTMS treatment, the system output was set to 110% of relaxed motor threshold and a repetition rate of 10 Hz. Stimulation was delivered in ten trains of 5 seconds each, with trains 30 seconds apart. The coil was oriented so that electric fields were induced to a sagittal plane. Ear protection was worn throughout.

Statistical Tests

Data were stored on a Lotus program. Comparisons on parametric and nonparametric variables were made by using Student's t-tests and chi-square tests, respectively.

RESULTS

Subjects

Fifty-six patients were recruited into the study, and 50 patients completed a course of 5 rTMS treatments. There were 21 responders (42%) and 29 nonresponders (58%; Table 2). Twenty-eight patients were less than age 65. Sixteen (56%) of these young patients responded to rTMS. However, only 5 (23%) of the 22 elderly (≥65 years of age) responded to rTMS (Table 2). Three of the 4 (75%) elderly depressed patients who had their first episode of depression prior to the age of 65 (early onset) responded to rTMS. However, only 2 (11%) of the 18 elderly patients with late-onset depression (first episode after the age of 65) responded to rTMS (Table 2). Individual scores fell by 60% or more in all responders and below 10 in 17 of the responders.
Patients who responded to rTMS differed significantly from those who did not respond with respect to age (P=0.038; Table 2) and pretreatment Ham-D scores (P=0.008). However, there was no difference in the pretreatment Ham-D scores between the young patients who responded to rTMS and those who did not. There was no gender difference between responders and nonresponders (P=0.5; Table 2). In addition, there was no significant difference in pre-rTMS MMSE scores between responders and nonresponders (P=0.2). Among patients with major depression (unipolar, recurrent), 17 of 39 (43.5%) were responders. Among patients with psychotic depression, 2 of 8 (25%) were responders (Table 2). Only 1 of 6 elderly patients with psychotic depression (17%) responded to rTMS. Two of 3 bipolar disorder patients (67%) and only 1 of 4 dementia patients (25%) responded to rTMS (Table 2). Sixteen patients reported a favorable response to ECT in the past; only 8 of these responded to rTMS. The only patient who reported an unfavorable response to ECT in the past likewise did not respond to rTMS.

Side Effects

Six of the 56 patients did not complete a course of rTMS. One 47-year-old man and a 33-year-old woman requested to stop after one rTMS treatment because of pain over the left frontal scalp area elicited during the treatment. In both cases, the pain stopped immediately with cessation of the rTMS treatment. Neither patient required an analgesic medication for the pain. A third patient was a 66-year-old man whose rTMS treatment was stopped because of brisk right upper extremity muscular contractions during the treatment. These muscular contractions ended immediately when the treatment was stopped. A fourth patient was a 44-year-old woman with preexisting motor tics of the right upper and lower extremity who had recurrence of these movements during her first rTMS treatment. Periodic limb flexion persisted for 20 minutes without change in speech or alertness; it could be quenched repeatedly with gentle pressure to the arm or leg. Movements ceased after 2 mg of lorazepam intravenously, without any subsequent complications. The fifth subject was a 45-year-old woman who developed a left body dysthesia 10 minutes after her first rTMS treatment. The dysthesia lasted approximately 48 hours and then resolved spontaneously. The patient's brain magnetic images, EEG, and neurologic examination were all within normal limits. Finally, a 77-year-old woman received one rTMS treatment without any complications. Six hours after her treatment she experienced a syncopal episode. Workup was negative, and the syncopal episode resolved without any complications. This patient did not experience any change in her blood pressure or heart rate during her rTMS treatment. It was not felt that the syncopal episode was related to the rTMS treatment. No patient developed a new onset of seizures during the course of rTMS. A 46-year-old woman, who was a responder to rTMS, initially reported that she had no history of epilepsy prior to beginning treatment. However, 2 weeks after starting treatment she reported apparent left focal motor seizures and admitted preexisting twitching of the left face. All episodes were remote from the times of rTMS by at least several hours. Complete neurological examination, EEG, and MRI were normal. Seizures continued despite therapeutic phenytoin levels and were highly correlated with attendance at church and funerals. After two episodes were witnessed in an outpatient psychiatry program, they were assessed as pseudoseizures. She was tapered off phenytoin without recurrence. Ten patients complained of mild headaches during the rTMS treatments. These headaches ended immediately after the treatments stopped. No patient required treatment with analgesics to control the headaches. All of these 10 patients completed their course of rTMS. No patients complained of any memory or cognitive side effects during rTMS. However, no formal cognitive testing was done in this study. rTMS had no effect on any patient's blood pressure or heart rate during the treatments.

DISCUSSION

The main finding of this study is that rTMS may be used safely and effectively in some patients with refractory depression. However, with the open-label design of this study, a placebo effect cannot be ruled out in the patients who responded to rTMS. In our study, 21 of 50 patients with depression (42%) responded to rTMS. In the largest rTMS study of depression to date, Pascual-Leone et al.9 reported that 11 of 17 depressed patients (65%) responded to rTMS. Consistent with the Pascual-Leone study, the majority of patients in our study were medication resistant. In fact, all but 3 of our patients had failed a 6-week trial of an antidepressant prior to receiving rTMS (Table 1).
Recently, Prudic et al.13 have reported that ECT may be less effective in patients who have not responded to a therapeutic trial of antidepressants pre-ECT. Given that nearly all of our patients had received a therapeutic trial of an antidepressant pre-rTMS, we were unable to examine the response rate from rTMS in a less refractory group of depressed patients. Clearly this is an area in need of further research.
The rTMS protocol used in our study was similar to that of Pascual-Leone et al.9 In both studies the therapeutic benefits of rTMS were observed after 5 rTMS treatments by stimulating the left prefrontal cortex. In addition, both studies used a frequency of 10 Hz. We used a higher magnetic field intensity (110% motor threshold) than was used in the Pascual-Leone study (90% motor threshold) and a shorter stimulus train with far fewer total pulses per session (500 vs. 2,000 pulses, 5 vs. 20 minutes). Clearly, additional placebo-controlled rTMS depression studies are required that examine the potential effects of different stimulus intensities, train durations, stimulus frequencies, number of treatment sessions, and anatomic stimulation sites on the therapeutic response from rTMS.
All of Pascual-Leone and colleagues' patients were under age 60, whereas in our study 22 of the subjects were 65 years of age or older. Interestingly, 16 of the younger patients (56%) responded to rTMS, whereas only 5 of the 22 elderly, depressed patients (23%) responded to rTMS. Furthermore, among the depressed elderly patients, 3 of the 4 (75%) who had their first episode of depression prior to age 65 (early onset) responded to rTMS, but only 2 of the 18 (11%) with late-onset depression (first episode after age 65) responded to rTMS. We have previously reported that there is an increased incidence of structural brain changes in elderly depressed patients and that elderly patients with late-onset depression have the most severe structural brain changes.14,15 These findings may explain the poor response from rTMS observed in our elderly depressed patients. At our institution, we are currently examining whether preexisting structural brain changes in the depressed elderly may predict a poor response from rTMS.
Consistent with Pascual-Leone's study, we did not find that a positive response to rTMS was related to the younger patients' Ham-D scores. In addition, there was no difference in gender or pre-rTMS MMSE scores between responders and nonresponders in this study. Sixteen patients reported a favorable response to ECT in the past. Of these, only 8 responded to rTMS. At our institution, we are currently examining whether nonresponders to rTMS are less likely to achieve a therapeutic response from ECT.
Although the antidepressant mechanisms of action for ECT and rTMS remain unknown, recent works are beginning to examine the neurochemical basis for rTMS and its effects on several animal behavioral models.1618 Both ECT and rTMS have been shown to reduce immobility in the forced swimming test. In addition, enhanced apomorphine-induced stereotypy was increased by both rTMS and ECT, implying a dopaminergic effect in both treatments. While rTMS is a nonconvulsive method for inducing depolarization of neurons in the brain, TMS has also been shown to inhibit seizure activity, decrease seizure duration, and increase the seizure threshold for additional ECT-induced seizures in animals; these findings are not unlike the anticonvulsant properties observed with ECT. Similar to ECT and antidepressants, rTMS may alter brain monoamines. Regional alterations in dopamine, serotonin, and 5-hydroxyindoleacetic acid levels have been reported with rTMS.
Finally, like antidepressants and ECT, rTMS can significantly decrease the number of beta-adrenergic receptors in certain parts of the rat's brain.18 On the basis of these works, it is not unreasonable to expect that further rTMS studies will enhance our understanding of the pathophysiology of depression and may ultimately lead to the development of safer, more effective treatments for depression.
In both Pascual-Leone's report and ours, no patient reported a new onset of seizures during rTMS treatments. However, in 2 patients during rTMS, muscular contractions spread from a single hand muscle to more proximal muscles in the right upper extremity. This may have represented intracortical spread of excitation. This spread of excitation in the primary motor cortex could be an indicator of the potential epileptogenicity of rTMS in individual patients.1 Neither of these individuals developed any neurologic sequelae. This spread of muscular excitation has been associated with higher frequencies of stimulation (≥5 Hz) during rTMS. Future rTMS research will be needed to examine the risks and benefits of high-frequency versus low-frequency rTMS treatments for depression. Headaches were the most common complaint; however, these were minor in most patients. Only 2 patients asked to discontinue rTMS because of the pain elicited during rTMS stimulation. There were no observed cardiovascular complications in any patients. This is of potential significance given the high incidence of preexisting coronary artery disease in many of our elderly patients.
Finally, none of our patients complained of memory or cognitive side effects from rTMS. These observations are consistent with previous safety reports on rTMS.1921 However, additional neuropsychological studies of rTMS are indicated to further examine this area.
In summary, rTMS appears to be safe and effective in treating some medication-resistant depressed patients. However, the therapeutic benefits of rTMS appear to be greater in younger patients. Future work is needed to examine ways to sustain the therapeutic benefits of rTMS and to identify the optimum techniques for its administration. The potential radiological and clinical predictors of response to rTMS will also need further study.
TABLE 1.
TABLE 2.

References

1.
George MS, Wassermann EM, Post RM: Transcranial magnetic stimulation: a neuropsychiatric tool for the 21st century. J Neuropsychiatry Clin Neurosci 1996; 8:373–382
2.
Pascual-Leone A, Catala MD, Pascual AP: Lateralized effect of rapid rate transcranial magnetic stimulation of the prefrontal cortex on mood. Neurology 1996; 46:499–502
3.
George MS, Wassermann EM, Williams WA, et al: Changes in mood and hormone levels after rapid-rate transcranial magnetic stimulation of the prefrontal cortex. J Neuropsychiatry Clin Neurosci 1996; 8:172–180
4.
George MS, Ketter TA, Post RM: Prefrontal cortex dysfunction in clinical depression. Depression 1994; 2:59–72
5.
Hoflich G, Kasper S, Hufnagel A, et al: Application of transcranial magnetic stimulation in treatment of drug-resistant major depression: a report of two cases. Human Psychopharmacology 1993; 8:361–365
6.
Grisaru N, Yarovslavsky U, Abarbanel J, et al: Transcranial magnetic stimulation in depression and schizophrenia. Eur Neuropsychopharmacol 1994; 4:287–288
7.
Kilbinger HM, Hoflich G, Hufnagel A, et al: Transcranial magnetic stimulation (TMS) in the treatment of major depression: a pilot study. Human Psychopharmacology 1995; 10:305–310
8.
George MS, Wassermann EM, Williams WA, et al: Daily repetitive transcranial magnetic stimulation (rTMS) improves mood in depression. NeuroReport 1995; 6:1853–1856
9.
Pascual-Leone A, Rubio B, Pallardo F, et al: Rapid-rate transcranial magnetic stimulation of left dorsolateral prefrontal cortex in drug-resistant depression. Lancet 1996; 348:233–237
10.
George MS, Wassermann EM, Williams WE, et al: Mood improvement following daily pre-frontal repetitive transcranial magnetic stimulation in patients with depression. Am J Psychiatry 1997; 154:1752–1756
11.
Sackeim HA, Decina P, Portnoy S, et al: Effects of electrode placement on the efficacy of titrated low-dosage ECT. Am J Psychiatry 1987; 144:1449–1455
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Epstein CM, Lah JK, Meador K, et al: Optimum stimulus parameters for lateralized suppression of speech with magnetic brain stimulation. Neurology 1996; 47:1590–1593
13.
Prudic J, Sackeim HA, Devanand DP: Medication resistance and clinical response to electroconvulsive therapy. Psychiatry Res 1990; 31:287–296
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Figiel GS, Krishnan KRR, Doraiswamy PM, et al: Subcortical hyperintensities on brain magnetic resonance imaging: a comparison between late age onset and early onset elderly depressed subjects. Neurobiol Aging 1991; 26:245–247
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Coffey CE, Wilkinson WE, Weiner RD, et al: Quantitative cerebral anatomy in depression. Arch Gen Psychiatry 1993; 50:7–16
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Fleischmann A, Prolov K, Abarbanel J, et al. The effect of transcranial magnetic stimulation of rat brain on behavioral models of depression. Brain Res 1995; 699:130–132
17.
Fleischmann A, Steppel J, Leon A, et al: The effect of transcranial magnetic stimulation compared with electroconvulsive shock on rat apomorphine-induced stereotypy. Eur Neuropsychopharmacol 1994; 4:449–450
18.
Klein E, Ben-Shachar D, Grisaru N, et al: Effects of rTMS on brain monoamines, receptors and animal models of depression. Presented to Biological Psychiatry Conference, San Diego, CA, May 1997
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Pascual-Leone A, Houser CM, Reeves K, et al: Safety of rapid-rate transcranial magnetic stimulation in normal volunteers. Electroencephalogr Clin Neurophysiol 1993; 89:120–130
20.
Wasserman EM, Grafman J, Berry C, et al: Use and safety of a new repetitive transcranial magnetic stimulator. Electroencephalogr Clin Neurophysiol (in press)
21.
Hufnagel A, Claus D, Brunhoelzl C, et al: Short-term memory: no evidence of effect of rapid-repetitive transcranial magnetic stimulation in healthy individuals. J Neurol 1993; 240:373–376

Information & Authors

Information

Published In

Go to The Journal of Neuropsychiatry and Clinical Neurosciences
Go to The Journal of Neuropsychiatry and Clinical Neurosciences
The Journal of Neuropsychiatry and Clinical Neurosciences
Pages: 20 - 25
PubMed: 9547462

History

Published in print: February 1998
Published online: 1 April 2006

Authors

Details

Gary S. Figiel, M.D.
Received July 16, 1997; revised and accepted October 8, 1997. From the Departments of Psychiatry and Neurology, Emory University School of Medicine, and Rehabilitation Research and Development Center, Atlanta VA Medical Center, Atlanta, Georgia. Address correspondence to Dr. Figiel, Emory Clinic at Wesley Woods Hospital, 1821 Clifton Rd., NE, Atlanta, GA 30329.
Charles Epstein, M.D.
Received July 16, 1997; revised and accepted October 8, 1997. From the Departments of Psychiatry and Neurology, Emory University School of Medicine, and Rehabilitation Research and Development Center, Atlanta VA Medical Center, Atlanta, Georgia. Address correspondence to Dr. Figiel, Emory Clinic at Wesley Woods Hospital, 1821 Clifton Rd., NE, Atlanta, GA 30329.
William M. McDonald, M.D.
Received July 16, 1997; revised and accepted October 8, 1997. From the Departments of Psychiatry and Neurology, Emory University School of Medicine, and Rehabilitation Research and Development Center, Atlanta VA Medical Center, Atlanta, Georgia. Address correspondence to Dr. Figiel, Emory Clinic at Wesley Woods Hospital, 1821 Clifton Rd., NE, Atlanta, GA 30329.
Jody Amazon-Leece, M.S., G.N.P.
Received July 16, 1997; revised and accepted October 8, 1997. From the Departments of Psychiatry and Neurology, Emory University School of Medicine, and Rehabilitation Research and Development Center, Atlanta VA Medical Center, Atlanta, Georgia. Address correspondence to Dr. Figiel, Emory Clinic at Wesley Woods Hospital, 1821 Clifton Rd., NE, Atlanta, GA 30329.
Linda Figiel, R.N., M.S.N.
Received July 16, 1997; revised and accepted October 8, 1997. From the Departments of Psychiatry and Neurology, Emory University School of Medicine, and Rehabilitation Research and Development Center, Atlanta VA Medical Center, Atlanta, Georgia. Address correspondence to Dr. Figiel, Emory Clinic at Wesley Woods Hospital, 1821 Clifton Rd., NE, Atlanta, GA 30329.
Aida Saldivia, M.D.
Received July 16, 1997; revised and accepted October 8, 1997. From the Departments of Psychiatry and Neurology, Emory University School of Medicine, and Rehabilitation Research and Development Center, Atlanta VA Medical Center, Atlanta, Georgia. Address correspondence to Dr. Figiel, Emory Clinic at Wesley Woods Hospital, 1821 Clifton Rd., NE, Atlanta, GA 30329.
Susan Glover, M.D.
Received July 16, 1997; revised and accepted October 8, 1997. From the Departments of Psychiatry and Neurology, Emory University School of Medicine, and Rehabilitation Research and Development Center, Atlanta VA Medical Center, Atlanta, Georgia. Address correspondence to Dr. Figiel, Emory Clinic at Wesley Woods Hospital, 1821 Clifton Rd., NE, Atlanta, GA 30329.

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