TADS study raises concerns -- Jureidini et al. 329 (7478): 1343 -- BMJ

Letter

TADS study raises concerns

EDITOR—We have additional concerns to those raised byLenzer about the adolescents with depression study (TADS).^1
2

TADS consists of two separate randomised studies: a double blindcomparison of fluoxetine (109 subjects) with placebo (112),and an unblinded comparison between cognitive behaviour therapyalone (111) and fluoxetine plus cognitive behaviour therapy(107). The lack of patient blinding and placebo control in thelatter group is likely to exaggerate the benefit seen in thefluoxetine plus cognitive behaviour therapy group, who receivemore face to face contact and know (as do their doctors) thatthey are not receiving placebo.

Comparing results across all four groups is therefore misleading.The authors' claim that a cognitive behaviour therapy plus placeboarm would have been both too expensive and too artificial tohave clinical relevance is unconvincing.

TADS found no statistical advantage of fluoxetine over placeboon the primary end point, the children's depression rating scale(CDRS-R; P = 0.10), but this was not mentioned in the abstract.This and the small or absent advantages of fluoxetine on otherend points (table) and in other studies,³ shows that fluoxetine,like all other antidepressants, is of doubtful clinical importancefor children.

View this table:
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Effect of fluoxetine and placebo on various end points

Adverse events and suicidal behaviour may be greater than theTADS paper says. Despite small numbers, more subjects leavingthe study than reporting adverse effects, and the splittingof adverse events into multiple groups, significantly more psychiatricadverse events occurred in the fluoxetine group than the placebogroup (² test (1 df), P = 0.047). Despite small numbers andthe exclusion of known suicidal behaviour, TADS found a trendto more suicidal behaviour (six attempts in the fluoxetine groupsand one attempt in the non-fluoxetine groups), consistent withother trials of selective serotonin reuptake inhibitors (SSRIs).We are less reassured than the authors by the fact that no attemptwas fatal. Suicide is a rare event so that a study the sizeof TADS should be expected to miss a significantly increasedrisk.

The data do not support the TADS authors' optimistic conclusions.The balance between benefit and harm of SSRI treatment for depressionin childhood and adolescence has yet to be shown to be favourable.

Jon Jureidini, head

Department of Psychological Medicine, Women's and Children's Hospital, North Adelaide 5006, Australia jureidinij@wch.sa.gov.au

Anne Tonkin, associate professor, department of clinical and experimental pharmacology, Peter R Mansfield, research fellow, department of general practice

University of Adelaide, Adelaide 5005, Australia

Additional authors are Peter Parry, child psychiatrist, Women'sand Children's Hospital, North Adelaide; David B Menkes, professorof psychological medicine, University of Wales Academic Unit,Wrexham; and Chris Doecke, associate professor of pharmacy practice,Quality Use of Medicines and Pharmacy Research Centre, Universityof South Australia, Adelaide.

Competing interests: None declared.

References

Lenzer J. Journalists on Prozac. BMJ 2004;329: 748. (25 September.)[Free Full Text]
Treatment for Adolescents with Depression Study Team. Fluoxetine, cognitive-behavioral therapy, and their combination for adolescents with depression: treatment for adolescents with depression study (TADS) randomized controlled trial. JAMA 2004;292: 807-20.[Abstract/Free Full Text]
Jureidini J, Doecke C, Mansfield P, Haby M, Menkes D, Tonkin A. Efficacy and safety of antidepressants for children and adolescents. BMJ 2004;328: 879-83.[Free Full Text]

Letter

TADS study raises concerns

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