Change in metabolic syndrome parameters with antipsychotic treatment in the CATIE Schizophrenia Trial: Prospective data from phase 1

Meyer, Jonathan M.; Davis, Vicki G.; Goff, Donald C.; McEvoy, Joseph P.; Nasrallah, Henry A.; Davis, Sonia M.; Rosenheck, Robert A.; Daumit, Gail L.; Hsiao, John; Swartz, Marvin S.; Stroup, T. Scott; Lieberman, Jeffrey A.

doi:10.1016/j.schres.2007.12.487

« Previous Next »Schizophrenia Research
Volume 101, Issue 1 , Pages 273-286, April 2008

Change in metabolic syndrome parameters with antipsychotic treatment in the CATIE Schizophrenia Trial: Prospective data from phase 1☆

Jonathan M. Meyer
- Department of Psychiatry, University of California, San Diego, United States
- VA San Diego Healthcare System, United Statess
- Corresponding author. San Diego VAMC, 3350 La Jolla Village Drive (116A), San Diego, CA 92161, United States. Tel.: +1 858 642 3570; fax: +1 858 552 7542.
Vicki G. Davis
- Department of Biostatistics, Collaborative Studies Coordinating Center, University of North Carolina at Chapel Hill, Bank of America Center, 137 E. Franklin Street, Suite 400, Chapel Hill, NC 27514-4145, United States
Donald C. Goff
- Department of Psychiatry, Harvard University, United States
- Schizophrenia Program, Massachusetts General Hospital, Freedom Trail Clinic, Lindemann Mental Health Center, 25 Staniford St., Boston, MA 02114, United States
Joseph P. McEvoy
- Department of Psychiatry and Behavioral Sciences, Duke University, United States
- Clinical Research, John Umstead Hospital, 1003 12th Street, Butner, NC 27509, United States
Henry A. Nasrallah
- Psychiatry and Neuroscience, University of Cincinnati, 231 Albert Sabin Way, PO Box 670559, Cincinnati, OH 45267-0559, United States
Sonia M. Davis
- Biostatistics, Quintiles Inc., 5927 South Miami Blvd, Morrisville, NC 27560, United States
Robert A. Rosenheck
- Epidemiology and Public Health, Yale Medical School, United States
- Child Study Center, Yale Medical School, United States
- Northeast Program Evaluation Center, VA Connecticut Health Care System, 950 Campbell Ave, West Haven, CT 06516, United States
Gail L. Daumit
- Epidemiology, and Health Policy and Management, Johns Hopkins Medical Institutions, 2024 East Monument Street, Suite 2-500, Baltimore, MD 21287, United States
John Hsiao
- Adult Psychopharmacology Intervention Program, National Institute of Mental Health, Bethesda, MD, United States
Marvin S. Swartz
- Department of Psychiatry and Behavioral Sciences, Duke University Medical Center, Box 3173, Duke University Medical Center, Durham, NC 27710, United States
T. Scott Stroup
- Department of Psychiatry, University of North Carolina at Chapel Hill, Campus Box 7160, Chapel Hill, NC 27599-7160, United States
Jeffrey A. Lieberman
- Department of Psychiatry, Columbia University, Psychiatric Institute, 1051 Riverside Drive, New York, NY 10032, United States

Received 1 September 2007; received in revised form 6 December 2007; accepted 22 December 2007. published online 13 February 2008.

Abstract

Background

The metabolic syndrome (MS) is associated with increased risk for diabetes mellitus and coronary heart disease, and is highly prevalent among schizophrenia patients. Given concerns over antipsychotic metabolic effects, this analysis explored MS status and outcomes in phase 1 of the CATIE Schizophrenia Trial.

Methods

The change in proportion of subjects with MS and individual criteria was compared between antipsychotic treatment groups, along with mean changes for individual criteria. Primary analyses examined subjects with fasting laboratory assessments at baseline and 3 months. Other analyses examined 3-month changes in MS status, waist circumference (WC), HDL cholesterol and blood pressure in all subjects, metabolic changes at the end of phase 1 participation (EOP), and repeated measures changes in HDL, blood pressure (BP) and WC over phase 1.

Results

At 3 months, there were no significant between-drug differences for the change in proportion of subjects meeting MS status or individual MS criteria in the smaller fasting cohort (n = 281) or for those meeting criteria for parameters not dependent on fasting status (BP, HDL, WC) among all subjects (n=660). Among all subjects whose MS status could be determined at 3 months (n=660), MS prevalence increased for olanzapine (from 34.8% to 43.9%), but decreased for ziprasidone (from 37.7% to 29.9%) (p=.001). Although effect sizes varied across subgroups, at 3 months olanzapine and quetiapine had the largest mean increase in waist circumference (0.7 in. for both) followed by risperidone (0.4 in.), compared to no change for ziprasidone (0.0 in.) and a decrease in waist circumference for perphenazine (−0.4 in.). Olanzapine also demonstrated significantly different changes in fasting triglycerides at 3 months (+21.5 mg/dl) compared to ziprasidone (−32.1 mg/dl). EOP exposure data was obtained, on average, nine months from baseline for all metabolic variables. Results from EOP and repeated measures analyses were consistent with those at 3 months for mean changes in WC and fasting triglycerides, but between group differences emerged for HDL and SBP.

Conclusions

This large non-industry sponsored study confirms the differential metabolic effects between antipsychotics. Clinicians are advised to monitor all metabolic parameters, including WC, HDL and serum triglycerides, during antipsychotic treatment.

Keywords: Antipsychotic, Schizophrenia, Metabolic syndrome, Lipids, HDL, Triglycerides, Waist circumference, Central adiposity