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Section of Neurochemical Imaging and Psychiatry, Institute of Psychiatry, De Crespigny Park, London SE5 8AF and Maudsley Hospital, London SE5 8AZ
Correspondence: E-mail: r.ohlsen{at}iop.kcl.ac.uk
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Abstract |
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To evaluate a psychosocial intervention for patients treated with antipsychotics with body mass index (BMI) >25. A total of 44 patients (mean age (s.e.) 37.6 (1.2); 28 female, 16 male) received dietary and exercise advice with motivational interviewing. Weight and BMI were measured at baseline and monthly thereafter. Patients were offered weight monitoring for 1 year.
RESULTS
Overall mean weight loss was 3.1 kg (mean 3.22%). Modal (range) weight change was -4.2 (-19.2 kg to +8.7 kg).
CLINICAL IMPLICATIONS
Overall weight loss was not significant after 355.7 (32.5) (mean, s.e.) days. Determinants of response remain unclear. Avoiding weight gain in the first instance is critical. Further research will explore determinants of antipsychotic-induced weight gain and prevention strategies.
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Introduction |
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Little data are available about the response of patients with schizophrenia who are overweight to psychosocial weight management interventions. We now evaluate such an intervention in overweight (body mass index (BMI) >25) individuals treated with antipsychotics.
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Method |
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We invited patients who were overweight, and wanted to lose weight, to participate in a weight management programme. Patients self-referred, or were referred to the service through their primary clinical teams. Patients were in- and out-patients of the South London and Maudsley National Health Service (NHS) Trust (catchment population 520 000).
The service inclusion criteria were: DSM-IV (American Psychiatric Association, 1994) diagnosis of schizophrenia, schizoaffective disorder or bipolar illness; stably maintained on antipsychotic treatment; overweight (BMI >25); and agreeable to participation in a weight management programme.
The exclusion criteria were: concomitant diagnosis of eating disorder, learning disability or substance misuse; and any physical problem (particularly cardiac) that might preclude participation in a weight management programme.
After screening, 44 patients were included. One patient did not meet the above criteria (BMI <25) but was included because of significant weight gain above her baseline (approximately 18 kg) and an abnormal waist-hip ratio. This patient was highly motivated to access the service.
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Treatment package |
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Results |
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To correct for this variation in time, and for the differing number of time points measured among individuals, data were converted into long clusters, imported from SPSS-10 into STATA-7 and regression analysis with robust standard errors performed. We found no significant change in weight overall. Furthermore, we failed to find any predictors of response.
Patients were on a variety of antipsychotic treatment, and some were also treated with mood stabilisers and antidepressants (Table 1). The majority were receiving clozapine or olanzapine. No relationship was found between the primary antipsychotic and weight change, nor did antidepressants or mood stabilisers affect outcome.
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Discussion |
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However, there was a wide variation in response to treatment (Fig. 1). Modest lifestyle changes and small weight losses (around 3 kg) prevented 58% of a population without psychoses (n=550) with impaired glucose tolerance (IGT) developing diabetes over a 5-year period (Tuomilehto et al, 2001). The mean weight loss for this group was 3.1kg. Though not statistically significant, such weight losses could have had some benefit by holding off incipient diabetes or IGT.
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Methodological considerations |
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Baseline weights before the start of antipsychotic treatment were unobtainable. Estimates of how much weight had actually been gained since the inception of antipsychotic treatment are unreliable. It is difficult to estimate how much weight these patients might have gained without intervention. Allison et al (1999) showed weight gains of 5.5 kg on clozapine and 4.5 kg on olanzapine after 10 weeks treatment; the patients in the study reported here were generally stabilised on their medication for longer periods of time. Patients who remained stable, or who gained weight, might have gained more weight without the intervention.
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Previous findings |
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At present we have no information that can explain the process of change. The patients who lost weight adhered to the prescribed diet, and exercised. Patients who gained weight or remained stable claimed to have followed the diet and exercise regimen also. We are planning a qualitative evaluation of the service using the Focus Group interview technique to uncover the elements of the programme that were helpful to some patients, and inform future service planning and delivery.
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Conclusions |
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Further research will investigate biological determinants of antipsychotic-induced weight gain (in particular pharmacogenetic and hormonal influences), identify high-risk groups and follow up the present cohort to determine longevity of response over time.
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Acknowledgments |
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References |
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