BMJ 2001;322:772-775 [Abridged] ( 31 March )

Primary care

Antidepressant drugs and generic counselling for treatment of major depression in primary care: randomised trial with patient preference arms

Editorial by Wagner and Simon

Clair Chilvers, professor aMichael Dewey, senior lecturer aKatherine Fielding, lecturer aVirginia Gretton, research assistant aPaul Miller, lecturer in health economics aBen Palmer, research associate aDavid Weller, professor cRichard Churchill, lecturer bIdris Williams, professor bNavjot Bedi, specialist registrar in psychiatry dConor Duggan, professor eAlan Lee, consultant psychiatrist and special senior lecturer fGlynn Harrison, professor g for the Counselling versus Antidepressants in Primary Care Study Group.

a Trent Institute for Health Services Research, University of Nottingham Medical School, Queen's Medical Centre, Nottingham NG7 2UH, b Division of General Practice, University of Nottingham Medical School, Queen's Medical Centre, c Department of General Practice, University of Edinburgh, 20 West Richmond St, Edinburgh EH8 9DX, d Division of Psychiatry, Nottingham Healthcare NHS Trust, Nottingham NG3 6AA, e Division of Forensic Mental Health, University of Leicester, Arnold Lodge, Leicester LE5 0LE, f Department of Psychiatry, University Hospital, Queen's Medical Centre, g Division of Psychiatry, University of Bristol, Bristol BS2 8DZ

Correspondence to: C Chilvers Clair.Chilvers{at}doh.gsi.gov.uk


    Abstract
Top
Abstract
Introduction
Participants and methods
Results
Discussion
References

Objectives: To compare the efficacy of antidepressant drugs and generic counselling for treating mild to moderate depression in general practice. To determine whether the outcomes were similar for patients with randomly allocated treatment and those expressing a treatment preference.
Design: Randomised controlled trial, with patient preference arms. Follow up at 8 weeks and 12 months and abstraction of GP case notes.
Setting: 31 general practices in Trent region.
Participants: Patients aged 18-70 who met research diagnostic criteria for major depression; 103 patients were randomised and 220 patients were recruited to the preference arms.
Main outcome measures: Difference in mean Beck depression inventory score; time to remission; global outcome assessed by a psychiatrist using all data sources; and research diagnostic criteria.
Results: At 12 months there was no difference between the mean Beck scores in the randomised arms. Combining the randomised and patient preference groups, the difference in Beck scores was 0.4 (95% confidence interval -2.7 to 3.5). Patients choosing counselling did better than those randomised to it (mean difference in Beck score 4.6, 0.0 to 9.2). There was no difference in the psychiatrist's overall assessment of outcome between any of the groups. 221/265(83%) of participants with a known outcome had a remission. Median time to remission was shorter in the group randomised to antidepressants than the other three groups (2 months v 3 months). 33/221 (15%) patients had a relapse.
Conclusions: Generic counselling seems to be as effective as antidepressant treatment for mild to moderate depressive illness, although patients receiving antidepressants may recover more quickly. General practitioners should allow patients to have their preferred treatment.


What is already known on this topic
Antidepressants and specific psychological interventions are effective in major depression.

Generic counselling has not previously been compared with antidepressants in primary care

What this study adds
12 months after starting treatment, generic counselling is as effective as antidepressants

Patients treated with antidepressants may recover more quickly

Given a choice, more patients opt for counselling

Patients who choose counselling may benefit more than those with no strong preference



    Introduction
Top
Abstract
Introduction
Participants and methods
Results
Discussion
References

Both antidepressants and psychological interventions have been shown to be effective in patients with major depression. 1 2 The counselling and antidepressants in primary care study was set up to compare the efficacy and cost effectiveness of antidepressant drugs and generic counselling in a naturalistic general practice setting. The short term outcomes from this study (at eight weeks) have been published.3 We report here the outcomes at 12 months.


    Participants and methods
Top
Abstract
Introduction
Participants and methods
Results
Discussion
References

Recruitment and treatment
Full details of the methods have been published.3 Briefly, we invited a random sample of 410 general practices in the Trent health region to enter patients into the trial. General practitioners recruited participants and obtained informed consent. Eligible patients were those aged 18-70 years who met the research diagnostic criteria (assessed by the general practitioner using a checklist) for major depression.4 We excluded patients with psychosis, suicidal tendencies, postnatal depression, a recent bereavement, or drug or alcohol misuse. The study was approved by 12 local research ethics committees.

For patients who agreed to randomisation, treatment was allocated by telephone with a randomisation strategy using blocks of four stratified by practice. Patients who refused randomisation but agreed to participate in the patient preference trial were given their choice of treatment. Treatment and follow up were identical in the randomised and patient preference groups.

We provided general practitioners with written guidelines on routine drug treatment of depression. Patients in the counselling arms were given six sessions by experienced counsellors, who adopted the counselling approach that they believed to be most suitable.

Data collection and follow up
All patients completed the Beck depression inventory5 and SF-36 questionnaire at enrolment. 6 7 At the follow up visits eight weeks and 12 months after enrolment, the general practitioner completed a form that included the research diagnostic criteria and the patient was asked to complete a form including the Beck depression inventory and SF-36. Patients who did not keep their follow up appointments were asked to complete the forms at home.

Outcome measures
The main outcome measures at 12 months were Beck depression inventory score, time to remission, 8 9 global outcome (classified as good, moderate, poor, or unknown), and research diagnostic criteria. Remission was defined as a score of less than 4 on the research diagnostic criteria, a Beck score of less than 10, or clear documentation in the general practitioner's notes that the patient was well. Relapse was defined as deterioration within six months of remission, and recurrence as deterioration after six months of remission.

Global outcome was assessed by a psychiatrist (NB) blind to treatment allocation using the research diagnostic criteria, Beck score, and general practitioners' notes. If the research diagnostic criteria and Beck scores were not available, global outcome was estimated from the case notes. The outcome was considered good if the patient responded to treatment within eight weeks and then remained well; moderate if the patient was slow to respond but then remained well or was well initially and then became unwell; and poor if the patient remained depressed throughout. The criteria for being well were the same as the criteria for remission.

Statistical analysis
We investigated differences in baseline characteristics and outcome measures between the groups using descriptive statistics, unpaired t tests, chi 2 tests, and Fisher's exact test. The analyses stratified by randomised or patient preference status used Mantel-Haenszel techniques. The time to remission was analysed by the Kaplan-Meier method, and differences were tested with the logrank test. 10 11

Based on a clinically important difference between the groups in mean Beck scores of 5 points, and assuming a standard deviation of 8.3 with two sided significance of 0.05, we required 44 patients per arm for power of 80% and 60 per arm for power of 90%.


    Results
Top
Abstract
Introduction
Participants and methods
Results
Discussion
References

Response rates
The figure shows the numbers of patients recruited and followed up. Sixty five (63%) patients in the randomised trial completed the Beck depression inventory and SF-36 at 12 months compared with 142 (65%) in the patient preference trial. The proportions of patients in each group who kept their 12 month appointment differed (P=0.01), with attendance ranging between 25% for patients choosing antidepressants and 53% for those randomised to antidepressants.



View larger version (33K):
[in this window]
[in a new window]
  		Recruitment and follow up of patients

We abstracted the general practitioner's notes for 96% (99/103) of patients in the randomised trial and 96% (212/220) in the patient preference. There was sufficient information to carry out the psychiatrist's overall assessment on 79% (81/103) of patients in the randomised trial and 74% (163/220) in the patient preference trial.

Patient characteristics at entry
The characteristics of randomised patients were comparable at baseline (table 1). Patients preferring counselling were less severely depressed than the randomised patients or those preferring antidepressants.3


                              
View this table:
[in this window]
[in a new window]
 

Table 1. Summary of baseline characteristics. Values are numbers (percentages) unless stated otherwise

Beck inventory scores at 12 months
Mean Beck scores did not differ significantly between the two groups in the randomised controlled trial (P=0.49, table 2). There was no evidence for an interaction between treatment and preference (P=0.6) so we combined the randomised and patient preference groups. Mean Beck scores were similar in counselled patients and those receiving antidepressants.


                              
View this table:
[in this window]
[in a new window]
 

Table 2. Scores on Beck depression inventory scale at 12 months

Global outcome and time to remission
We found no differences in global outcome between the randomised or patient preference trials when outcome was split into good or moderate versus poor (table 3). Stratification by randomised or patient preference status gave similar outcomes for antidepressants and counselling (Mantel Haenszel P=0.63).


                              
View this table:
[in this window]
[in a new window]
 

Table 3. Global outcome, remission, and relapse in randomised and patient preference groups. Values are numbers (percentages) of patients. Totals exclude missing data but include patients in whom outcome was uncertain

Research diagnostic criteria scores
Of the randomised patients who kept their 12 month follow up, nine (47%) in the counselling group were no longer depressed compared with 21 (78%) in the antidepressant group (P=0.07). When we assumed that all those failing to attend had recovered, then 81% in the counselling group and 88% in the antidepressant group were no longer depressed. The figures when we assumed that patients failing to attend were treatment failures were 17% and 41% respectively (P=0.01).

In the patient preference trial, 48 (80%) patients choosing counselling and 17 (85%) choosing antidepressants had recovered at 12 months (P=0.87). If missed appointments were assumed to be treatment successes the outcomes were similar, but if all missed appointments were treatment failures, patients choosing counselling would do better than those choosing antidepressants.


    Discussion
Top
Abstract
Introduction
Participants and methods
Results
Discussion
References

The data from our randomised controlled trial suggest that at 12 months follow up generic counselling and antidepressants are equally effective in patients with mild to moderate depression; remission rates are impressive with both treatments. Patients treated with antidepressants recovered more quickly than those receiving counselling. Choice of treatment seemed to be beneficial, but this applied only to counselling. This finding should be treated with caution as the power of the study to detect interactions was low.

The larger numbers of patients choosing counselling in this trial suggests that patients prefer counselling to antidepressants.3 A survey of people attending general practice had similar findings.12

Several caveats must be taken into account when interpreting these data. Firstly, we had difficulty recruiting patients into the randomised controlled trial. The patient preference arms, although increasing the power of the study, tend to make our findings less robust. Secondly, the counselling offered in the study was of a high standard; patients were referred within two weeks, and all the counsellors were experienced. Thirdly, although we found some benefit associated with choice, we did not investigate the effect of giving an alternative treatment to those with a specific preference.

What conclusions should commissioners and general practitioners draw from this study? Firstly, that both counselling and antidepressant drugs are effective, but antidepressants may result in more rapid recovery. Secondly, that given the choice more patients with depression will choose counselling and those who choose antidepressants are likely to be more severely depressed. We recommend that general practitioners should allow patients to have their choice of treatment. However, if the patient does not have a preference, antidepressant drugs should be prescribed because counselling is a scarce resource that is best reserved for those patients who express a preference for it.

    Acknowledgments

We thank Helen Bounds and Joanne Elliott for secretarial and clerical support and Paddy Hawtin for help with data collection. We thank the general practitioners who recruited the patients for this study, and the patients who participated.

Contributors: CC, MD, CD, KF, GH, AL, DW, and IW developed the study protocol. RC, VG, DW, and IW recruited the practices. VG carried out the fieldwork with clinical support from RC. NB, CD, and AL reviewed the case notes and global outcomes. BP, MD, and PM carried out the data analysis. CC wrote the paper, and all authors commented on the drafts. CC and CD are the guarantors.

    Footnotes

Funding: NHS Executive Trent.

Competing interests: None declared.

The full version of this paper appears on the BMJ's website


    References
Top
Abstract
Introduction
Participants and methods
Results
Discussion
References

1. American Psychiatric Association. Practice guidelines for major depressive disorder in adults. Am J Psychiatry 1993; 150(suppl): 4.
2. Churchill R, Dewey M, Gretton V, Duggan C, Chilvers C, Lee AS. Should general practitioners refer patients with major depression to counsellors? A review of current published evidence. Br J Gen Pract 1999; 49: 737-743.
3. Counselling versus Antidepressants in Primary Care Study Group. Assessing treatment effectiveness in depression: results from a PRPT trial. Br J Psychiatry 2000; 177: 312-318[Abstract/Full Text].
4. Spitzer RL, Endicot J, Robins E. Research diagnostic criteria: rationale and reliability. Arch Gen Psychiatry 1978; 35: 773-782[Medline].
5. Beck AT, Ward CH, Mendelson M, Mock J, Erbaugh J. An inventory for measuring depression. Arch Gen Psychiatry 1961; 4: 561-571.
6. Brazier JE, Harper R, Jones NMB, O'Cathain A, Thomas KJ, Usherwood T, et al. Validating the SF-36 health survey questionnaire: new outcome measure for primary care. BMJ 1992; 305: 160-164[Medline].
7. Jenkinson C, Coulter A, Wright L. Short form 36 (SF-36) health survey questionnaire: normative data for adults of working age. BMJ 1993; 306: 1437-1440[Medline].
8. Paykel ES, Priest RG, on behalf of conference participants. Recognition and management of depression in general practice: consensus statement. BMJ 1992; 305: 1198-1202[Medline].
9. Frank E. Response, remission, recovery, relapse, recurrence. J Clin Psychiatry 1991; 52(suppl 2): 2-16.
10. Kaplan EL, Meier P. Nonparametric estimation from incomplete observations. J Am Stat Assoc 1958; 53: 457-481.
11. Mantel N, Haenszel P. Statistical aspects of the analysis of data from retrospective studies of disease. J Natl Cancer Inst 1959; 22: 719-748.
12. Churchill R, Khaira M, Gretton V, Chilvers C, Dewey M, Duggan C, et al. Treating depression in general practice: factors affecting patients' treatment preferences. Br J Gen Pract 2000; 50: 905-906[Medline].

(Accepted 1 December 2000)

© BMJ 2001
Add to CiteULike CiteULike   Add to Complore Complore   Add to Connotea Connotea   Add to Del.icio.us Del.icio.us   Add to Digg Digg   Add to Reddit Reddit   Add to Technorati Technorati    What's this?

Related Articles

Systematic review to determine whether participation in a trial influences outcome
Gunn Elisabeth Vist, Kåre Birger Hagen, P J Devereaux, Dianne Bryant, Doris Tove Kristoffersen, and Andrew David Oxman
BMJ 2005 330: 1175. [Abstract] [Full Text] [PDF]

Antidepressants and counselling for major depression in primary care
Wai-Ching Leung, Andrew Martyn Thornett, David Curtis, Clair Chilvers, and Michael Dewey
BMJ 2001 323: 282. [Extract] [Full Text]

Black dog
BMJ 2001 322: 0. [Full Text] [PDF]

Black dog
BMJ 2001 322: 0. [Full Text] [PDF]

GPs should let depressed patients choose treatment method
BMJ 2001 322: 0. [Full Text]

Managing depression in primary care
Edward H Wagner and Gregory E Simon
BMJ 2001 322: 746-747. [Extract] [Full Text] [PDF]

This article has been cited by other articles:

  • Dobscha, S. K., Corson, K., Gerrity, M. S. (2007). Depression Treatment Preferences of VA Primary Care Patients. Psychosomatics 48: 482-488 [Abstract] [Full text]  
  • Pollock, K. (2007). Maintaining face in the presentation of depression: constraining the therapeutic potential of the consultation. Health (London) 11: 163-180 [Abstract]  
  • HOWARD, L., THORNICROFT, G. (2006). Patient preference randomised controlled trials in mental health research. Br. J. Psychiatry 188: 303-304 [Abstract] [Full text]  
  • Gum, A. M., Arean, P. A., Hunkeler, E., Tang, L., Katon, W., Hitchcock, P., Steffens, D. C., Dickens, J., Unutzer, J., for the IMPACT Investigators, (2006). Depression Treatment Preferences in Older Primary Care Patients. Gerontologist 46: 14-22 [Abstract] [Full text]  
  • Vist, G. E., Hagen, K. B., Devereaux, P J, Bryant, D., Kristoffersen, D. T., Oxman, A. D. (2005). Systematic review to determine whether participation in a trial influences outcome. BMJ 330: 1175- [Abstract] [Full text]  
  • King, M., Nazareth, I., Lampe, F., Bower, P., Chandler, M., Morou, M., Sibbald, B., Lai, R. (2005). Impact of Participant and Physician Intervention Preferences on Randomized Trials: A Systematic Review. JAMA 293: 1089-1099 [Abstract] [Full text]  
  • Chisholm, D., Sanderson, K., Ayuso-Mateos, J. L., Saxena, S. (2004). Reducing the global burden of depression: Population-level analysis of intervention cost-effectiveness in 14 world regions. Br. J. Psychiatry 184: 393-403 [Abstract] [Full text]  
  • Lawrie, I., Lloyd-Williams, M., Taylor, F. (2004). How do palliative medicine physicians assess and manage depression. Palliat Med 18: 234-238 [Abstract]  
  • Lloyd-Williams, M. (2003). Depression--the hidden symptom in advanced cancer. JRSM 96: 577-581 [Full text]  
  • (2003). Mild depression in general practice: time for a rethink?. DTB 41: 60-64 [Abstract] [Full text]  
  • Bower, P., Byford, S., Barber, J., Beecham, J., Simpson, S., Friedli, K., Corney, R., King, M., Harvey, I. (2003). Meta-analysis of data on costs from trials of counselling in primary care: using individual patient data to overcome sample size limitations in economic analyses. BMJ 326: 1247-1250 [Abstract] [Full text]  
  • DUGGAN, C., MILTON, J., EGAN, V., McCARTHY, L., PALMER, B., LEE, A. (2003). Theories of general personality and mental disorder. Br. J. Psychiatry 182 : s19-s23 [Abstract] [Full text]  
  • Raine, R., Haines, A., Sensky, T., Hutchings, A., Larkin, K., Black, N. (2002). Systematic review of mental health interventions for patients with common somatic symptoms: can research evidence from secondary care be extrapolated to primary care?. BMJ 325: 1082-1082 [Abstract] [Full text]  
  • Leung, W.-C., Thornett, A. M., Curtis, D., Chilvers, C., Dewey, M. (2001). Antidepressants and counselling for major depression in primary care. BMJ 323: 282-282 [Full text]  
  • Wagner, E. H, Simon, G. E (2001). Managing depression in primary care. BMJ 322: 746-747 [Full text]  
  • Barkham, M., Hardy, G. E (2001). Counselling and interpersonal therapies for depression: towards securing an evidence-base. Br Med Bull 57: 115-132 [Abstract] [Full text]  

Rapid Responses:

Read all Rapid Responses

Improving preference measurement in primary care studies.
Andrew Martyn Thornett
bmj.com, 31 Mar 2001 [Full text]
Author’s conclusions were not justified by findings
Wai-Ching Leung
bmj.com, 1 Apr 2001 [Full text]
Doubtful 12 month intervention effects
Christopher Dowrick
bmj.com, 2 Apr 2001 [Full text]
Depression requires a multidimensional approach to managment
Steve Williams
bmj.com, 3 Apr 2001 [Full text]
Two distinct anti-depression treatments used together
Salvador Vale
bmj.com, 5 Apr 2001 [Full text]
further analysis
Arthur Rifkin
bmj.com, 13 Apr 2001 [Full text]
The type of treatment matters less than ensuring it is done properly and followed up
David Simpson
bmj.com, 30 Apr 2001 [Full text]
Does randomization introduce bias?
Toke S Barfod
bmj.com, 10 May 2001 [Full text]

Student BMJ

Risk of surgery for inflammatory bowel disease: record linkage studies

What can you learn from this BMJ paper? Read Leanne Tite's Paper+

www.student.bmj.com

Listen to the latest BMJ Interview