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Prognostic value of frontal functional neuroimaging in late-onset severe major depression

Published online by Cambridge University Press:  02 January 2018

Víctor Navarro*
Affiliation:
Clinical Institute of Psychiatry and Psychology, Hospital Clinic, Barcelona, Spain
Cristóbal Gastó
Affiliation:
Department of Nuclear Medicine, Hospital Clinic, Barcelona, Spain
Francisco Lomeña
Affiliation:
Clinical Institute of Psychiatry and Psychology, Hospital Clinic, Barcelona
Xavier Torres
Affiliation:
Department of Nuclear Medicine, Hospital Clinic
José J. Mateos
Affiliation:
Clinical Institute of Psychiatry and Psychology Hospital Clinic, Barcelona, Spain
María Portella
Affiliation:
Clinical Institute of Psychiatry and Psychology Hospital Clinic, Barcelona, Spain
Guillem Masana
Affiliation:
Clinical Institute of Psychiatry and Psychology Hospital Clinic, Barcelona, Spain
Teodoro Marcos
Affiliation:
Clinical Institute of Psychiatry and Psychology Hospital Clinic, Barcelona, Spain
*
Dr Víctor Navarro, Hospital Clinic, Departamento de Psiquiatría, Villarroel 170, 08036 Barcelona, Spain. Tel: 343 2275477; fax: 343 2275477; e-mail: [email protected]
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Extract

Background

There is growing evidence of a relationship between frontal neuroimaging and neuropsychological abnormalities and the physiopathology and course of late-onset major depression.

Aims

To assess acute antidepressant response in late-onset major depression in relation to baseline frontal perfusion ratios.

Method

A 99mTc HMPAO single photon emission computed tomographic brain scan was performed in medication-free patients with late-onset major depression, who were then included in a 12-week antidepressant treatment regimen. Logistic regression was used to define a predictive model of non-remission.

Results

Atotal of 47 patients completed the study 34 of whom were classed as remitters and 13 as non-remitters. The variable left anterior fronto-cerebellar perfusion ratio had a global predictive power of 87%. Analysing this variable together with the baseline variables age of onset and duration of index episode, the predictive power of the model rose to 94%.

Conclusions

Our study suggests that a specific frontal functioning could predict the acute antidepressant response in late-onset severe major depression.

Type
Papers
Copyright
Copyright © Royal College of Psychiatrists, 2004 

Neuropsychological studies (Reference Alexopoulos, Meyers and YoungAlexopoulos et al, 2000), structural neuroimaging studies (Reference Alexopoulos, Kiosses and ChoiAlexopoulos et al, 2002) and functional neuroimaging studies (Reference Kumar, Thomas and LavretskyKumar et al, 2002; Reference Navarro, Gastó and LomeñaNavarro et al, 2002) have suggested the possible involvement of the frontal lobes in the physiopathology of late-onset major depression. Various structural neuroimaging studies have stressed the possible influence of these frontal alterations on the course of the disorder (Reference Simpson, Baldwin and JacksonSimpson et al, 1998; Reference Alexopoulos, Kiosses and ChoiAlexopoulos et al, 2002). To our knowledge, no prognostic study as yet has used functional neuroimaging. Following on from the vascular depression concept defined by Alexopoulos et al (Reference Alexopoulos, Meyers and Young1997), the hypothesis we put forward here is that the greater the frontal hypoperfusion, the poorer the clinical evolution of late-onset major depression. After establishing in an earlier study (Reference Navarro, Gastó and LomeñaNavarro et al, 2002) that perfusion abnormalities detected during active depression in elderly patients in the left anterior frontal region disappeared in remission, the main aim of our study was to assess in a new sample the acute response to antidepressant medication of patients with late-onset major depression in relation to baseline frontal perfusion ratios.

METHOD

Sample

The study was conducted at the Hospital Clínic of Barcelona. Participants were recruited from in-patients and out-patients with a diagnosis of major depressive disorder, aged 60 years or over; all were right-handed. Only people with late-onset depression were included, i.e. those in whom depression had begun after the age of 50. To be eligible for inclusion, patients had to fulfil the DSM–IV (American Psychiatric Association, 1994) criteria for a current major depressive episode. We excluded patients with neurological disorders, those receiving medications with potential central nervous system side-effects and those with uncontrolled medical illness at the time of recruitment. Psychiatric exclusion criteria included any history of mania, hypomania or non-affective psychosis, and current substance dependence. Similarly, in order to reduce the risk that prior exposure to electroconvulsive therapy (ECT) might bias the results, we excluded patients who had received ECT within 6 months of recruitment.

The study was approved by the ethical committee of our hospital. All patients (or a close relative when there was doubt about the patient's understanding) gave informed written consent.

Clinical assessment

Depressive symptoms were rated on the Spanish version of the 17-item Hamilton Rating Scale for Depression (HRSD; Reference HamiltonHamilton, 1960; Reference Ramos-Brieva and Cordero-VillafafilaRamos-Brieva & Cordero-Villafafila, 1988) and on the Newcastle Scale (Reference Carney, Roth and GarsideCarney et al, 1965). All patients recruited had a baseline HRSD score of 21 or greater. A baseline Newcastle Scale score of 7 or higher was used to define endogenous depression. We also screened for reduced global cognitive function using the Spanish version of the Mini-Mental State Examination (MMSE; Reference Folstein, Folstein and McHughFolstein et al, 1975; Reference Lobo, Saz and MarcosLobo et al, 1999).

Following Baldwin & Tomenson (Reference Baldwin and Tomenson1995), we quantified vascular risk factors as follows: 0, absent; 1, mild (asymptomatic), for example, controlled hypertension or clinical evidence of arteriosclerosis (e.g. carotid murmur); 2, moderate (symptomatic), for example, poorly controlled hypertension, symptomatic angina or history of myocardial infarction; and 3, severe (active disease), for example, peripheral vascular disease with amputation or transient ischaemic attack. Other vascular risk factors such as blood levels of cholesterol and glucose were also assessed.

Study design

To minimise bias from the administration of psychotropic drugs, patients underwent a minimum washout period of 10 days for antidepressant medication and a minimum of 2 days for benzodiazepine medication. Baseline clinical assessments, including brain single photon emission computed tomography (SPECT), were then conducted. After the SPECT scan, treatment was started. Fortnightly clinical evaluations (HRSD) were made during the study. Evaluators were masked to the functional neuroimaging measures. Patients were considered to be in remission when the 17-item HRSD score was below 8 on two consecutive visits.

Treatment protocol

The treatment used complied with standard therapeutic norms, and specifically with our hospital's treatment protocol for elderly patients with major depression. The antidepressant initially used was nortriptyline at a daily dosage of 12.5 mg, which was raised to 25 mg and then 50 mg on the fourth and eighth day of treatment, respectively. Nortriptyline plasma concentrations were determined after 1 week of stable dosing; the dose was adjusted to obtain a blood level between 80 ng/ml and 120 ng/ml (304–456 nmol/l); maximum dose 100 mg/day. All patients achieved correct plasma levels during the first month of treatment. In combination with antidepressant treatment, both haloperidol (up to 4 mg/day for management of psychotic symptoms) and lorazepam (up to 4 mg/day for management of anxiety/insomnia) were allowed.

Patients remained on a regimen of nortriptyline for 12 weeks. Patients whose HRSD score had not fallen by at least 50% by the end of the sixth week of nortriptyline treatment received adjunctive citalopram (20 mg/day) until the end of the 12-week follow-up.

SPECT procedure

At the end of the drug wash-out period, each participant underwent a 99m-technetium hexamethylpropylene amine oxime (99mTc-HMPAO) SPECT brain scan. The scan was performed using a rotating dual-head gamma camera (Helix, General Electric Medical Systems), fitted with a high-resolution fanbeam collimator. Data acquisition started 20 min after intravenous injection of 740 MBq 99mTc-HMPAO (Ceretec; Nycomed, Amersham, UK). Sixty 30 s frames were collected in a 360° circular orbit, step and shoot mode, using a 128 × 128 matrix.

Image data were processed on an Elscint SP1 computer (Apex SP-X, software version 3.12). Reconstruction was performed by filtered back-projection using a Metz filter (power factor 3). No attenuation correction was performed. The final pixel size was 3.9 mm and the full width at half-maximum in the transaxial plane was 10 mm. Semi-quantitative regional cerebral blood flow analysis was performed using irregular regions of interest (ROIs) stored in the computer as a T 1-weighted magnetic resonance imaging (MRI) template. Brain SPECT images were normalised to the standard T 1-weighted MRI. The ROIs were placed in ten 7.8-mm-thick oblique slices, which were parallel to the fronto-cerebellar plane. For each hemisphere, anterior fronto-cerebellar ratios were obtained as 100 × mean counts per pixel of anterior frontal ROIs divided by the mean counts per pixel of cerebellar ROIs. Using the same formula, the posterior fronto-cerebellar ratios were also obtained. The nuclear medicine physician was masked to the 12-week course.

Statistical procedures

Comparisons between groups were assessed by using the Student's t-test (or the Mann–Whitney U-test for non-parametric data) for continuous variables and the chi-squared test for discrete variables. The Kolmogorov–Smirnov test was applied to assess the normality of the continuous variables. The level of statistical significance was set at P<0.05.

Logistic regression methods were used to define a predictive model of non-remission. In the first stage, only the frontal perfusion measures were assessed. In the second stage, the baseline functional neuroimaging variables and the baseline clinical and demographic variables were assessed jointly to improve the model. Different models were obtained and explored by forward selection, backward selection and stepwise regression. The most significant variables were then fixed in the model and the others were introduced progressively to improve the adjustment. The model calibration was assessed by the Hosmer–Lemeshow goodness-of-fit test. Finally, the reliability and precision of each model were analysed in order to choose the best final solution (Reference DoménechDoménech, 1999).

To avoid any possible separation between groups confounding the results, the predictive models were assessed further by using a split-half approach. To try to avoid an unlucky splitting of the samples that would cause some variables to be absent in certain groups, the following approach was adopted. The whole sample was split randomly into two groups, A and B. To increase the possibility that the data-sets to be analysed covered the complete variation, two more groups were generated, C and D. Group C was made from the first half of A and B, and group D from the last half of A and B. Every model was fitted to each of the data-sets. If the solution replicates over sets A and B or over sets C and D, the possibility of empirical verification of correctness of the solution (i.e. that the model captures essential variation not only pertaining to the specific samples) is increased. By contrast, although the absence of stability of some components across subsamples might reflect its presence only in specific subsets, this finding increases the probability that the model will not be valid.

Finally, for further clarification of our findings in a clinical sense, the receiver operating characteristic (ROC) curve was measured for each continuous variable to define the cut-off point with the best sensitivity and specificity.

RESULTS

The initial sample comprised 52 patients, five of whom were eventually excluded: one had died, two did not attend scheduled follow-up visits, and two required ECT because of severe clinical deterioration. The final sample therefore comprised 47 patients.

The Kolmogorov–Smirnov test showed that three variables (MMSE score, Newcastle Scale score and the previous evolution in years) did not adjust to a normal distribution. It was possible to calculate a logarithmic transformation of the Newcastle score for adjustment to a normal distribution. It was not possible to transform the MMSE score or the years of previous evolution for adjustment to a normal distribution.

The mean age was 74.28 (s.d.=7.68, range 62–89) years. Approximately two-thirds of patients were female (68%). Patients’ symptoms were moderate to severe, as shown by their HRSD scores (mean 31.04, s.d.=6.25) and by the incidence rates of endogenous features (32%), psychotic features (19%) and admissions to hospital (23%).

Of the 47 patients who completed the study, 34 were classed as ‘remitters’ and 13 as ‘non-remitters’. Some clinical data for both subgroups are presented in Table 1. Significant differences between the subgroups were found in the variables duration of current episode, Newcastle score, left anterior frontal ratio (LAFR) and right anterior frontal ratio. No significant difference was found in other clinical variables such as age of onset, age of index episode or presence of vascular risk factors, or in neuroimaging variables such as left and right posterior frontal ratios (Table 1).

Table 1 Baseline demographic, clinical and neuroimaging characteristics of study sample

Variable Remitters (n=34) Non-remitters (n=13) Statistic d.f. P
χ2 t Z
Gender (n (%)) 0.65 1 0.42
     Female 22 (65) 10 (77)
     Male 12 (35) 3 (23)
Age, years (mean (s.d.)) 74.50 (7.52) 73.69 (8.38) 0.32 45 0.75
Vascular risk factor (n (%)) -0.46 NA 0.65
     Absent 10 (29) 1 (8)
     Mild 9 (26) 7 (54)
     Moderate 15 (44) 5 (38)
Cholesterol level, mg/dl (mean (s.d.)) 176.22 (29.73) 182.63 (35.47) 0.53 45 0.63
Glucose level, mg/dl (mean (s.d.)) 82.15 (13.63) 87.70 (14.1) 1.25 45 0.22
HRSD score (mean (s.d.)) 30.79 (6.61) 31.69 (5.36) 0.44 45 0.66
MMSE score (mean (s.d.)) 27.12 (1.09) 27.38 (0.87) -1.13 NA 0.26
Newcastle Scale score (mean (s.d.)) 6.50 (2.08) 5.23 (1.09) 2.36 33.541 0.022
Psychotic features (n (%)) 0.16 1 0.68
     Yes 7 (21) 2 (15)
     No 27 (79) 11 (85)
Endogenous features (n (%)) 2.26 1 0.13
     Yes 13 (38) 2 (15)
     No 21 (62) 11 (85)
Treatment regimen (n (%)) 0.64 1 0.42
     In-patient 9 (27) 2 (15)
     Out-patient 25 (74) 11 (85)
Age at onset, years (mean (s.d.)) 71.97 (7.18) 70.69 (6.47) 0.56 45 0.58
Previous depression (n (%)) 0.23 1 0.63
     Recurrent 13 (38) 4 (31)
     Single episode 21 (62) 9 (69)
Previous evolution, years (mean (s.d.)) 2.35 (3.46) 2.77 (4.92) -0.07 NA 0.94
Current episode duration, months (mean (s.d.)) 2.74 (1.56) 4.46 (1.98) 3.14 45 0.003
Fronto-cerebellar perfusion ratios (mean (s.d.))
     Left anterior ratio 93.35 (2.43) 98.32 (1.91) 6.61 45 <0.001
     Right anterior ratio 97.10 (2.60) 99.02 (2.48) 2.30 45 0.03
     Left posterior ratio 90.50 (4.20) 91.92 (4.96) 0.99 45 0.33
     Right posterior ratio 92.29 (3.97) 93.05 (5.95) 0.51 45 0.61

Predictive model of non-remission with frontal perfusion measures

Of the four frontal areas assessed (left and right anterior frontal and left and right posterior frontal) the predictive model included only the LAFR (Wald χ2=11.88; d.f.=1, P<0.01). The model explained 67.8% of the proportion of uncertainty of data (–2lnR=25.65; χ2=29.78; d.f.=1; P<0.01; Nagelkerke R 2=0.678). Its goodness of fit was acceptable (χ2=2.66; d.f.=7; P<0.92) and the predictions showed good sensitivity (76.9%) and specificity (91.2%). The global predictive power was 87.2%. The inclusion of the LAFR indicated that the risk of non-remission at 3-month follow-up rose almost 2.5 times with every point that the LAFR increased (exp(B)=2.54; 95% CI 1.5–4.32). In the split-half approach, the only variable entering the four subsamples was the LAFR. The solution was found to be replicated over subsets (Table 2).

Table 2 Split-half analysis of the predictive model of non-remission with SPECT variables (LAFR)

Model statistics Variable statistics
χ2 d.f. P -2lnR Nagelkerke R 2 Wald χ2 d.f. P Change -2lnR d.f. P
Group A 15.54 1 <0.001 11.45 0.71 4.84 1 0.03 15.54 1 <0.001
Group B 15.75 1 <0.001 12.52 0.70 5.51 1 0.02 15.75 1 <0.001
Group C 5.67 1 0.02 8.1 0.48 3.9 1 0.08 5.67 1 0.02
Group D 17.78 1 <0.001 14.06 0.72 7.06 1 <0.01 17.78 1 <0.001

The ROC curve measurement for the LAFR showed that the best cut-off point was a ratio value of 95.5 (sensitivity 92.3%; specificity 88.2%); area under the curve=0.95; 95% CI 0.89–1; P<0.01).

Global predictive model of non-remission

To improve the predictive model, the second stage assessed both the baseline functional neuroimaging variables and the baseline clinical and demographic variables. The global predictive model included LAFR (Wald χ2=6; d.f.=1; P<0.01), current episode duration (Wald χ2=4.57; d.f.=1, P=0.03) and current age (Wald χ2=3.31; d.f.=1; P=0.07). Although statistically non-significant, current age increased the proportion of uncertainty explained by the model significantly (75% to 83%) and in particular improved the Hosmer–Lemeshow goodness of fit (χ2 significance from P=0.58 to P=0.99). Although lacking clinical significance, current age was finally included for methodological adjustment. This global model explained 83% of the proportion of uncertainty of data (–2lnR=15.08; χ2=40.35; d.f.=3; P=0.01; Nagelkerke R 2=0.832), its goodness of fit was appropriate (χ2=0.96; d.f.=7; P=0.99) and its predictions showed good sensitivity (92.3%) and specificity (94.1%). The global predictive power was 93.6%.

The most determinant variable was the LAFR. The risk of non-remission at 3-month follow-up rose almost sixfold for each point that the LAFR increased (exp(B)=5.65; 95% CI 1.41–22.61). The second variable entering the final model was the current episode duration, indicating that the risk of non-remission increased almost fourfold for every extra month in the current episode duration (exp(B)=3.81; 3.81; 95% CI 1.12–12.93). In the split-half approach, the only variable entering the four subsamples was again the LAFR. The solution including the clinical variables was not replicated over subsets (Table 3).

Table 3 Split-half analysis of the global predictive model of non-remission

Model statistics Variable statistics
χ2 d.f. P -2lnR Nagelkerke R 2 Wald χ2 d.f. P Change -2lnR d.f. P
Group A 15.54 1 <0.001 11.45 0.71
     LAFR 4.84 1 0.03 15.54 1 <0.001
Group B 22.2 2 <0.001 6.06 0.87
     LAFR 1.44 1 0.23 17.91 1 <0.001
     Newcastle 1.12 1 0.29 6.46 1 0.01
Group C 5.67 1 0.02 8.1 0.48
     LAFR 3.9 1 0.08 5.67 1 0.02
Group D 24.22 2 <0.001 7.62 0.87
     LAFR 3.17 1 0.07 11.66 1 0.001
     Current episode duration 1.49 1 0.22 6.44 1 0.01

The best cut-off point for current episode duration according to the ROC curve measurement was 2.5 months (sensitivity 84.6%; specificity 55.9%; area under the curve=0.76; 95% CI 0.61–0.9; P=0.007).

DISCUSSION

The main findings of this study are that:

  1. (a) The LAFR seems to be able to predict response to acute pharmacological treatment in late-onset major depression.

  2. (b) Adding baseline clinical variables, duration of index episode and current age to the LAFR in the statistical analysis seems to increase the model's predictive power. However, these results are not confirmed by the split-half approach, and could be due to the sample characteristics.

Variables predicting outcome

Our results suggest that the risk of non-remission at 3-month follow-up increases almost 2.5 times with each extra point in the LAFR. The cut-off point of 95.5 predicts with an acceptable sensitivity and specificity the remission/non-remission of the depressive episode after 3 months of pharmacological treatment. Unlike structural neuroimaging studies of patients with late-onset major depression, which have described an association between frontal structural alterations and response to treatment (Reference Simpson, Baldwin and JacksonSimpson et al, 1998; Reference Alexopoulos, Kiosses and ChoiAlexopoulos et al, 2002), to our knowledge this is the first functional neuroimaging study to report an association between cerebral perfusion and response to pharmacological treatment in this subgroup of patients with depression. The stability of the SPECT variable for predicting the therapeutic outcome across the split-half approach increases the possibility of correctness of the model.

Furthermore, in our study, the addition of the duration of the index episode and current age seemed to increase the model's predictive ability. However, taking into account that these results were not confirmed in the split-half approach, the absence of stability of some clinical components across subgroups increases the probability that the model will not be valid and challenges the conclusions obtained from its use. In either case, further studies applying the same models on an entirely different data-set are required to confirm our findings.

The possible association between the clinical variables, duration of index episode and current age, and course of the illness has been assessed in a number of studies, but the results are inconsistent. Like us, a number of authors have found a correlation between older age at the time of the index episode and poor response to treatment (Reference Kennedy, Kelman and ThomasKennedy et al, 1991; Reference Dew, Reynolds and HouckDew et al, 1997), although the results of other studies have not corroborated this claim (Reference Burvill, Hall and StampferBurvill et al, 1991; Reference TumaTuma, 1996; Reference Halloran, Prentice and MurrayHalloran et al, 1999; Reference Bosworth, Hays and GeorgeBosworth et al, 2002). Equally, our finding of a correlation between longer duration of current episode and poorer response to treatment is in agreement with some earlier studies (Reference MurphyMurphy, 1983; Reference TumaTuma, 1996; Reference Halloran, Prentice and MurrayHalloran et al, 1999), but not with others (Reference Burvill, Hall and StampferBurvill et al, 1991; Reference Kennedy, Kelman and ThomasKennedy et al, 1991; Reference Dew, Reynolds and HouckDew et al, 1997; Reference Bosworth, Hays and GeorgeBosworth et al, 2002). This lack of consensus is probably caused by the wide range of methodological approaches, statistical analyses and demographic characteristics of the samples in these studies.

Regarding other clinical variables, it should be emphasised that the existence of significant differences in the Newcastle Scale scores between remitters and non-remitters (higher scores among remitters; Table 1) seems consistent with most of the previous studies suggesting higher rates of response to acute anti-depressive treatment in patients with endogenous depression compared with patients with non-endogenous depression (Reference Nelson and CharneyNelson & Charney, 1980; Reference SchatzbergSchatzberg, 1999). At this point, it is not possible to know whether increasing the size of our study sample would have incorporated the Newcastle clinical variable in the global predictive model.

Significance of frontal perfusion abnormalities in late-onset major depression

It is not easy to explain why the lower the LAFR (i.e. the higher the left anterior frontal hypoperfusion) the better the rates of clinical remission. It could be that the LAFR reflects only the speed of response to pharmacological treatment and not remission/non-remission. A longer follow-up of the patients, especially bearing in mind the evidence that geriatric patients might take longer to respond to anti-depressant treatment (Reference Mulsant and PollockMulsant & Pollock, 1998; Reference Reynolds, Frank and KupferReynolds et al, 1996), would provide more information on this issue. It is difficult to establish the histological and clinical significance of the cut-off point described; in any case, we believe that its significance lies in its usefulness as a prognostic factor and as a variable in the area of research.

We should stress that the direction of the prediction is at the very least surprising, especially as the few descriptive studies using functional neuroimaging to investigate acute major depression in the elderly have obtained inconsistent results (Reference Ebmeier, Glabus and PrenticeEbmeier et al, 1998; Reference Halloran, Prentice and MurrayHalloran et al, 1999; Reference Navarro, Gastó and LomeñaNavarro et al, 2002). These inconsistencies suggest that the alterations in frontal perfusion in this disorder are not specific.

The frontal functioning neuroimaging results of our study do not support our initial hypothesis and therefore do not corroborate the proposal of Alexopoulos et al (Reference Alexopoulos, Meyers and Young1997) of a degenerative ischaemic process as the cause of late-onset major depression (vascular depression). Our hypothesis was that the greater the frontal hypoperfusion (supposedly a manifestation of cerebral ischaemia), the lower would be the level of clinical reversibility (that is, a lower rate of remitters). This study found the reverse to be the case.

To explain this unexpected result, we could state that most studies of vascular depression are associative (Reference O'Brien, Desmond and AmesO’Brien et al, 1996; Reference Greenwald, Kramer-Ginsberg and KrishnanGreenwald et al, 1998) rather than causative, and it is possible that the frequently observed association between late-onset major depression and vascular disease could in fact be the result of unknown confounding factors. A vascular aetiology has been proposed for late-onset depression on the strength of the presence of hyperintensities, although the physiopathological bases of these lesions have not been determined definitively in patients with major depression (Reference Thomas, O'Brien and DavidThomas et al, 2002). We should add that this is not the first study to obtain results that challenge the degenerative vascular hypothesis for late-onset major depression (Reference Dupont, Butters and SchaferDupont et al, 1995; Reference Ebmeier, Prentice and RymanEbmeier et al, 1997; Reference Greenwald, Kramer-Ginsberg and KrishnanGreenwald et al, 1998; Reference Navarro, Gastó and LomeñaNavarro et al, 2002). Nonetheless, we should stress that the inferences made in this section, i.e. that our results do not support the vascular depression hypothesis, are based on the possible but unproven association between brain SPECT alteration and ischaemia. This association is debatable, given the absence of conclusive studies that support its existence in major depression.

Our results suggest that the pattern of left anterior frontal perfusion reflects a primary alteration of neuronal activity, probably reversible, and that there might not necessarily be a primary vascular substrate. Equally, although future studies should test the predictive models obtained here, this report provides strong evidence in favour of the existence of specific neuro-functional predictors of the course in late-onset severe major depression.

Clinical Implications and Limitations

CLINICAL IMPLICATIONS

  1. The presence of a high level of left anterior frontal perfusion suggests poor acute antidepressant response in late-onset severe major depression.

  2. The frontal lobes, especially the left anterior frontal area, seem to be linked to the physiopathology of late-onset severe major depression.

  3. The relationship between late-onset major depression and vascular depression is an important issue of which little is known at present.

LIMITATIONS

  1. As this is a study of predictive factors, a larger sample size would have been desirable.

  2. Only patients with late-onset and severe depression were included in our sample, meaning that the results cannot be extrapolated to the general population or even to the general elderly population.

  3. Treatment was administered in a naturalistic manner.

Footnotes

Declaration of interest

None.

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Figure 0

Table 1 Baseline demographic, clinical and neuroimaging characteristics of study sample

Figure 1

Table 2 Split-half analysis of the predictive model of non-remission with SPECT variables (LAFR)

Figure 2

Table 3 Split-half analysis of the global predictive model of non-remission

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