Full Text (PDF) Alert me when this article is cited Alert me if a correction is posted Citation Map Email this article to a Colleague Similar articles in this journal Similar articles in PubMed Alert me to new issues of the journal Add to My Articles & Searches Download to citation manager Citing Articles via HighWire Citing Articles via Google Scholar Articles by LINDENMAYER, j.–P. Articles by PATEL, R. Search for Related Content PubMed Citation Articles by LINDENMAYER, j.–P. Articles by PATEL, R. Schizophrenia Spectrum Disorders Other Neuroleptics

Olanzapine-Induced Ketoacidosis With Diabetes Mellitus

To the Editor: Olanzapine is a new atypical antipsychotic compound with a receptor profile similar to that of cloza­pine, with generally few side effects. Specifically, extrapyramidal symptoms did not change in relation to baseline when olanzapine-treated patients and control subjects were compared (1–3), although weight gain and transient liver enzyme elevation have been found. Given olanzapine's structural similarity to clozapine, it might be expected that some rare side effects seen with clozapine, such as impairment of glucose tolerance, could occur with olanzapine (4). We report on a patient who developed acute ketoacidosis with diabetes mellitus while taking olanzapine.

Mr. A was a 50-year-old, single, African American man with a 30-year psychiatric history with multiple psychiatric hospitalizations. He had been admitted to Manhattan Psychiatric Center 20 years earlier and had been hospitalized continuously since then. His diagnoses included schizophrenia (paranoid type), substance dependence, and antisocial personality disorder. He had a significant history of criminal and deviant sexual behavior. His medical history included hypertension, mild obesity (227 lb), and myocardial infarction but not diabetes. He had been on a regimen of extended-release nifedipine, 30 mg/day, to control his hypertension. He did not have a significant family history of diabetes.

During Mr. A's hospitalization, a variety of anti­psychotic medications were used, including fluphenazine decanoate, 25 to 75 mg i.m. every 2 weeks, chlorpromazine, 1800 mg/day, and haloperidol, 40 mg/day. He had no major side effects from these drugs. Mr. A had also received divalproex sodium, 750 mg twice a day, for 2 years. His psychiatric disorder had remained resistant to conventional antipsychotic medications. He refused to take clozapine because of the blood testing that was required. The results of his annual laboratory tests in 1997, including his blood sugar level, were normal.

Mr. A started olanzapine treatment, 5 mg/day. He continued to receive fluphenazine decanoate, 75 mg i.m. every 2 weeks, and divalproex sodium, 750 mg twice a day. His olanzapine dose was then gradually titrated to 30 mg/day over 6 months with the intent of gradually tapering his dose of fluphenazine decanoate once he was stable. His delusions and paranoid symptoms improved with this therapy. His weight was 227 lb at the start of olanzapine treatment, it increased to 248 lb after 5 months, and then it went down to 205 lb at the end of treatment. That same month, Mr. A was found drowsy, lethargic, and unresponsive to verbal commands. His blood pressure was 98/68 mm Hg, and he had orthostatic hypotension. Mr. A was then transferred to a hospital emergency room and later admitted to the intensive care unit for diabetic ketoacidosis; he had a blood sugar level of 1200 mg/dl. He was given intravenous insulin and 5% dextrose fluid.

Mr. A's olanzapine regimen was discontinued, and his diabetic ketoacidosis disappeared. He received human insulin (NPH), 40 to 70 units for 15 days. His insulin treatment was then discontinued, with subsequent normalization of his blood sugar level. His levels of blood sugar, urine sugar, and acetone remained normal. He remained on a regimen of fluphenazine decanoate, 75 mg i.m. every 2 weeks, benztropine mesylate, 2 mg twice a day, and divalproex sodium, 750 mg twice a day. Both the manufacturer of olanzapine and the Food and Drug Administration's MedWatch were notified of his drug reaction.

Mr. A developed de novo diabetes mellitus after 8 months of adjunctive olanzapine treatment. After he discontinued olanzapine, his diabetes mellitus disappeared completely. We believe that olanzapine constituted an etiological factor in the development of Mr. A's endocrine disorder. According to the manufacturer of olanzapine, diabetes mellitus was reported in 0.6% of patients in olanzapine premarketing trials (G. Rubel, Eli Lilly and Co., personal communication). As with clozapine, the pathophysiology of decreased glucose tolerance is unknown. Weight gain during olanzapine treatment is well recognized and may have contributed to the development of Mr. A's vulnerability to diabetes mellitus. Furthermore, he did not have a family history of diabetes mellitus. It is also possible that the 6 weeks of his high dose of olanzapine (30 mg/day) may have played a role, although it is not clear at what drug level the first symptoms of impaired glucose tolerance appeared. Also, it cannot be ruled out that the combination of olanzapine, fluphenazine decanoate, and divalproex sodium may have had an adverse effect on Mr. A's glucose tolerance. However, he had been taking fluphenazine decanoate and divalproex sodium for several months before the onset of his diabetes mellitus and again after recovery from it, without diabetic symptoms. Olanzapine or one of its metabolites may have contributed to the suppression of insulin release. This effect has been reported in studies with chlorpromazine, another anti­psychotic, which can produce a hyperglycemic response in rats during in vivo and in vitro studies (5). Clinicians using olanzapine at a dose of more than 20 mg/day in patients developing symptoms of diabetes mellitus or in patients with a preestablished history of diabetes mellitus may need to check blood sugar levels more frequently.

REFERENCES

1. Beasley CM Jr, Tollefson G, Tran P, Satterlee W, Sanger T, Hamilton S: Olanzapine versus placebo and haloperidol: acute phase results of the North American double-blind olanzapine trial. Neuropsychopharmacology 1996; 14:111–123[Medline]
2. Tollefson GD, Beasley CM Jr, Tran PV, Street JS, Krueger JA, Tamura RN, Graffeo KA, Thieme ME: Olanzapine versus haloperidol in the treatment of schizophrenia and schizoaffective and schizophreniform disorders: results of an international collaborative trial. Am J Psychiatry 1997; 154:457–465[Abstract]
3. Beasley CM Jr, Sanger T, Satterlee W, Tollefson G, Tran P, Hamilton S: Olanzapine versus placebo: results of a double-blind, fixed-dose olanzapine trial. Psychopharmacology (Berl) 1996; 124:159–167[Medline]
4. Popli AP, Konicki PE, Jurjus GJ, Fuller MA, Jaskiw GE: Clozapine and associated diabetes mellitus. J Clin Psychiatry 1997; 58:108–111[Medline]
5. Ammon HPT, Orci L, Steinke J: Effect of chlorpromazine (CPZ) on insulin release in vivo and in vitro in the rat. J Pharmacol Exp Ther 1973; 187:423–429[Abstract/Free Full Text]

This article has been cited by other articles:

				W. S. Stone and L. J. Seidman Toward a Model of Memory Enhancement in Schizophrenia: Glucose Administration and Hippocampal Function Schizophr Bull, January 1, 2008; 34(1): 93 - 108. [Abstract] [Full Text] [PDF]

				M. K. Varma, K. Connolly, and B. Fulton Life-Threatening Hyperglycemia and Acidosis Related to Olanzapine: A Case Report and Review of the Literature J Intensive Care Med, January 1, 2007; 22(1): 52 - 55. [Abstract] [PDF]

				M. Olfson, S. C. Marcus, P. Corey-Lisle, A.V. Tuomari, P. Hines, and G. J. L'Italien Hyperlipidemia Following Treatment With Antipsychotic Medications Am J Psychiatry, October 1, 2006; 163(10): 1821 - 1825. [Abstract] [Full Text] [PDF]

				B. L. Lambert, F. E. Cunningham, D. R. Miller, G. W. Dalack, and K. Hur Diabetes Risk Associated with Use of Olanzapine, Quetiapine, and Risperidone in Veterans Health Administration Patients with Schizophrenia Am. J. Epidemiol., October 1, 2006; 164(7): 672 - 681. [Abstract] [Full Text] [PDF]

				A. R. Fulbright and K. T. Breedlove Complete Resolution of Olanzapine-Induced Diabetic Ketoacidosis Journal of Pharmacy Practice, August 1, 2006; 19(4): 255 - 258. [Abstract] [PDF]

				R. B. Zipursky, H. Gu, A. I. Green, D. O. Perkins, M. F. Tohen, J. P. McEvoy, S. M. Strakowski, T. Sharma, R. S. Kahn, R. E. Gur, et al. Course and predictors of weight gain in people with first-episode psychosis treated with olanzapine or haloperidol The British Journal of Psychiatry, December 1, 2005; 187(6): 537 - 543. [Abstract] [Full Text] [PDF]

				C. Bushe and C. Paton The potential impact of antipsychotics on lipids in schizophrenia: is there enough evidence to confirm a link? J Psychopharmacol, November 1, 2005; 19(6_suppl): 76 - 83. [Abstract] [PDF]

				J.-P. Lindenmayer, P. Czobor, J. Volavka, L. Citrome, B. Sheitman, J. P. McEvoy, T. B. Cooper, M. Chakos, and J. A. Lieberman Changes in Glucose and Cholesterol Levels in Patients With Schizophrenia Treated With Typical or Atypical Antipsychotics Am J Psychiatry, February 1, 2003; 160(2): 290 - 296. [Abstract] [Full Text] [PDF]

				C. E. Koro, D. O. Fedder, G. J. L'Italien, S. Weiss, L. S. Magder, J. Kreyenbuhl, D. Revicki, and R. W. Buchanan An Assessment of the Independent Effects of Olanzapine and Risperidone Exposure on the Risk of Hyperlipidemia in Schizophrenic Patients Arch Gen Psychiatry, November 1, 2002; 59(11): 1021 - 1026. [Abstract] [Full Text] [PDF]

				C. E Koro, D. O Fedder, G. J L'Italien, S. S Weiss, L. S Magder, J. Kreyenbuhl, D. A Revicki, and R. W Buchanan Assessment of independent effect of olanzapine and risperidone on risk of diabetes among patients with schizophrenia: population based nested case-control study BMJ, August 3, 2002; 325(7358): 243 - 243. [Abstract] [Full Text] [PDF]

				D. Straker, A. Mendelowitz, and L. Karlin Near Fatal Ketoacidosis With Olanzapine Treatment Psychosomatics, August 1, 2002; 43(4): 339 - 340. [Full Text]

				J. W. Newcomer, D. W. Haupt, R. Fucetola, A. K. Melson, J. A. Schweiger, B. P. Cooper, and G. Selke Abnormalities in Glucose Regulation During Antipsychotic Treatment of Schizophrenia Arch Gen Psychiatry, April 1, 2002; 59(4): 337 - 345. [Abstract] [Full Text] [PDF]

				K. Melkersson and A.-L. Hulting Recovery From New-Onset Diabetes in a Schizophrenic Man After Withdrawal of Olanzapine Psychosomatics, February 1, 2002; 43(1): 67 - 70. [Full Text]

				R. P. JOHNSON, M. T. AL-TAHER, L. E. MADLOCK, M. GUO, and C. S. NASDAHL Increasing Insulin Dose for Olanzapine-Related Diabetes Am J Psychiatry, January 1, 2002; 159(1): 150 - 151. [Full Text] [PDF]

				B. C. Lund, P. J. Perry, J. M. Brooks, and S. Arndt Clozapine Use in Patients With Schizophrenia and the Risk of Diabetes, Hyperlipidemia, and Hypertension: A Claims-Based Approach Arch Gen Psychiatry, December 1, 2001; 58(12): 1172 - 1176. [Abstract] [Full Text] [PDF]

				B. Luna and M. N. Feinglos Drug-Induced Hyperglycemia JAMA, October 24, 2001; 286(16): 1945 - 1948. [Full Text] [PDF]

Full Text (PDF) Alert me when this article is cited Alert me if a correction is posted Citation Map Email this article to a Colleague Similar articles in this journal Similar articles in PubMed Alert me to new issues of the journal Add to My Articles & Searches Download to citation manager Citing Articles via HighWire Citing Articles via Google Scholar Articles by LINDENMAYER, j.–P. Articles by PATEL, R. Search for Related Content PubMed Citation Articles by LINDENMAYER, j.–P. Articles by PATEL, R. Schizophrenia Spectrum Disorders Other Neuroleptics

Get information about faster international access.

Privacy Policy

Copyright © 1999 American Psychiatric Association. All rights reserved.

Home | Search | Current Issue | Past Issues | Subscribe | All APPI Journals | Help | Contact Us