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Pharmacopsychiatry 2001; 34(6): 223-231
DOI: 10.1055/s-2001-18034
DOI: 10.1055/s-2001-18034
Original Paper
© Georg Thieme Verlag Stuttgart · New YorkEndocrine and Metabolic Abnormalities Involved in Obesity
Associated with Typical Antipsychotic Drug Administration
Further Information
Publication History
Publication Date:
26 October 2001 (online)
In this study, the authors assessed the endocrine system and glucose tolerance in obese and non-obese women chronically treated with typical antipsychotic drugs (AP). In particular, we tested the hypotheses that these subjects display hypogonadism and increased insulin resistance compared to healthy weight-matched controls, as these abnormalities create a tendency towards excessive body weight gain. Twenty-six AP-treated women were matched with 26 healthy women by age, body mass index and day of the menstrual cycle. The following serum variables were evaluated in each subject: glucose tolerance after an oral glucose overload, insulin, leptin, β-endorphin, reproductive hormones, adrenal steroids and lipids. Compared to controls, AP-treated women displayed significantly higher levels of basal glucose, insulin after 60 min of the glucose overload, prolactin, thyroid stimulating hormone and β-endorphin, with lower levels of C-Peptide, progesterone, 17-OH progesterone, androstenedione and high-density lipoprotein cholesterol. The levels of estradiol, estrone and leptin did not differ between the groups. Thus, women treated with typical AP appeared to display more insulin resistance than healthy controls, predisposing them to excessive weight gain. Insulin sensitivity might be further impaired when the subject switches to atypical AP administration. Metformin and related agents may reduce body weight in these subjects. The high levels of the opiate β-endorphin suggest that opiate antagonists such as naloxone and naltrexone might be useful as well. Even though the luteal phase of the menstrual cycle appears to be severely disturbed, the normal serum levels of estradiol and estrone do not support the proposal derived from animal experimental studies about the use of estrogens or tamoxifen to counteract AP-induced obesity.
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Trino BaptistaM.D.
Douglas Hospital Research Center (F1116)
6875 Lasalle Blvd
Verdun
Quebec, Canada H4H 1R3
Phone: (514) 761 61 31 ext. 34 52
Fax: (514) 888 40 64
Email: baptri@douglas.mcgill.ca