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- Clin Psychopharmacol Neurosci
- v.17(1); 2019 Feb
- PMC6361044
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Clin Psychopharmacol Neurosci. 2019 Feb; 17(1): 130–133.
Published online 2019 Feb 28. doi:10.9758/cpn.2019.17.1.130
PMCID: PMC6361044
PMID: 30690949
Hyun-Sic Jo,1 Sheng-Min Wang,1,2 and Jung Jin Kim
1
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Abstract
Phentermine is a sympathomimetic amine, like amphetamine, which is one of the most often prescribed drugs for weight loss. Although exact mechanism of phentermine causing psychosis is still not clear, numerous reports already showed that phentermine can induce psychosis. Psychotic symptoms are generally resolved once the medications are stopped. In contrast, we present a case of a 25-years-old Asian female patient who developed psychotic symptoms repeatedly after phentermine administrations. This case suggests that phentermine can cause psychotic episodes repeatedly, resulting in chronic occupational and social impairment. Therefore, a precautious measure such as government regulations for physicians prescribing and an education for patients taking phentermine are urgently needed.
Keywords: Phentermine, Adverse reaction, Psychotic disorders, Recurrence
INTRODUCTION
2014 Korean National Health Survey showed that 31.5% of Koreans over 19 years old are obese defined by World Health Organization Western Pacific Regional Office criteria (obese: body mass index [BMI] higher than 25 kg/m2). The obesity rate of general population in Korea was 26.0% in 1998, which has risen to 31–33% since 2007.1) Diet modification, exercise, and life style change are recommended as the first-line treatments of obesity.2) However, effects of lifestyle intervention are not always satisfactory, so several medications were tried and thus approved by the United States Food and Drug Administration (FDA) for obesity. Pharmacotherapy is indicated in individuals with a BMI of ≥25 kg/m2, or those with a BMI of ≥23 kg/m2 and having comorbidities such as hypertension, dyslipidemia, type 2 diabetes mellitus, or sleep apnea.3) Korea is world known for being an “appearance-obsessed” country, so many young females use or sometimes abuse “diet pills” to lose their weight. In terms of using diet pills and appetite suppressants, Korea ranks near the top of the globe. A research showed that up to 13% of female aged 15 to 59 years used or were using diet pills.4) FDA-approved anti-obesity drugs are orilistat, lorcaserin, phentermine/topiramate, naltrexone/bupropion and liraglutide.5)
Phentermine, which was approved in 1959 for weight loss, remains the most often prescribed drug for weight loss in the United States.6) Phentermine was approved for short-terms uses only, which is widely interpreted as up to 12 weeks, and its usual dose is 37.5 mg/day.2,6) It is sym-pathomimetic amines, like amphetamine, which is non-selective stimulator of synaptic noradrenaline, dopamine, and serotonin release. However, unlike amphetamine, it has very little effect on dopamine release at the neuronal synapse.5,7) The introduction of phentermine to Korea was much later than that of the United States. However, it has become the most widely used diet pills since its approval in 2004.5,8) According to a report by the Ministry of Food and Drug Safety, production performance of phentermine in Korea was 19,795 million Korean won (KRW; about 17 million dollars) in 2010, 43,553 million KRW (about 38 million dollars) in 2014, and 38,878 million KRW (about 34 million dollars) in 2015.9)
Like many other sympathomimetics, phentermine is known to induce psychotic symptoms. Thus, phentermine associated psychotic symptoms have been reported repeatedly since 1960s.10) Once the medications are stopped, psychotic symptoms generally improve in patients who had no prior history of psychotic disorder. Here we report a 25 years old woman whose psychotic symptoms recurred multiple times after re-administration of phentermine.
CASE
A 25-year-old Korean female patient was admitted to an acute psychiatric ward in April 2016 due to psychotic symptoms. A detailed mental status examination showed persecutory delusion, delusion of reference and auditory hallucination which occurred 6 weeks before admission. History revealed that she became pre-occupied with her body image from time to time. Thus, she has been taking diet pills and have presented with psychotic symptoms multiple times in the past. She first started taking diet pills in April 2011 from a medical clinic nearby. The medications included Furimin tablet® (phentermine 37.5 mg; Alvogen Korea, Seoul, Korea), L-Carina tablet® (330 mg; Alvogen Korea), Aeiol tablet® (alginic acid 200 mg, carboxymethyl-cellulose 100 mg; Pharvis Korea, Seoul, Korea), Therrmofen-S tablet® (acetaminophen 200 mg, caffeine 40 mg, ephedrine 15 mg; Alvogen Korea). She first took these medications irregularly and often developed idea of reference. She often avoided social interaction, such as refusing to participate in a group project at her college classes, but these symptoms did not cause significant problems.
She started to overdose phentermine (112.5–150.0 mg/day) from November 2012, which was immediately after she broke up with her boyfriend. Three to four weeks later, she displayed psychotic symptoms including persecutory delusion and delusion of reference, so she was not able to attend school and had to take a year of sick leave from her college. She was recommended to take anti-psychotics by a psychiatrist in a primary neuropsychiatric clinic, but she refused to do so. Thereafter, she stopped taking phentermine, and her psychotic symptoms subsided 3 weeks after phentermine cessation.
After returning to her school in February 2014, she became pre-occupied with her body image once again. As a result, she started re-taking phentermine irregularly and showed idea of reference from time to time. Her use of phentermine became regular from early 2015 which progressed to taking four times its recommended dosage of 150 mg/day from 2 months before admission. Shortly after, she started to feel that her coworkers were constantly watching her and trying to physically abuse her. She also started having auditory hallucinations; voices of her parents criticizing her about taking phentermine. She also became violent and threat to her own safety. Thus, she was hospitalized to our psychiatric ward by her legal guardian.
On admission, her affect was slightly tense, and she complained of delusion of reference, persecutory delusion, and inappropriate guilt. Her BMI was 23 kg/m2 (height, 163 cm; weight, 61 kg), and she was preoccupied with her body weight. Initial Positive and Negative Syndrome Scale (PANSS) score was 95. She had no previous neuropsychiatric history, history of physical illness, and family history of psychiatric illness. She did not have any suicidal ideation or attempt. Results of routine laboratory tests were normal. She was tested positive only for ephedrine on the urine drug screening.
We diagnosed her with substance-induced psychotic disorder because she never experienced psychotic symptoms before she took the diet pills. Among diet pills she had taken, ephedrine and caffeine may also induce psychosis. However, very few cases report ephedrine or caffeine induced psychosis episodes. In addition, the dosage of ephedrine and caffeine that she took was very low to induced psychosis.11,12) In contrast, it is well known that overdose or continuous use of phentermine can cause psychotic symptoms.13) Therefore, we concluded that phentermine was the most likely cause of her psychotic symptoms.
We prescribed her antipsychotic because her psychotic symptoms persisted although she had stopped taking the diet pills from 3 days before admission. We chose aripiprazole because it has less risk of causing weight gain.14,15) Additionally, we prescribed her lorazepam and benztropine. We increased aripiprazole to 15 mg on the 4th day of admission. After the 8th day of admission, her delusion subsided substantially, and she interacted appropriately within the psychiatric ward. Moreover, she started having insight about her symptoms and realized the risk of overdosing phentermine. Her symptoms improved gradually, and she was discharged on the 28th day of admission. On discharge, her PANSS score was dramatically improved to 20. She has been following up at our outpatient clinic without relapse of any psychotic symptom.
DISCUSSION
Phentermine has been known as an effective appetite suppressant with weight reduction effect.16,17) Phentermine is a substrate-type releaser at norepinephrine and dopamine transporters, with less potent effects at serotonin in the brain.18) These actions of phentermine may contribute to anti-appetite effect. Although side effects of phentermine have been generally tolerable,8) it can cause tachycardia, hypertension, visual symptoms, nausea, insomnia and anxiety.19) Moreover, phentermine may be associated with affective symptoms including manic-like episode.20)
Our case showed that patients may experience repeated psychotic episodes with phentermine administration. To the best of our knowledge, there was only one previous case report which showed recurrence of psychotic symptoms after phentermine administration.21) In our case, she stared experiencing mild psychotic symptoms when she first took phentermine intermittently, and the psychotic symptoms resolved without any treatment after she stopped taking it. Psychotic symptoms relapsed and aggravated when she started re-taking phentermine, more frequently and excessively.
Although exact mechanism of phentermine causing psychosis is still not clear, numerous reports already showed phentermine induced psychosis.13,21–25) A number of amphetamine related drugs including phentermine are known as antiobesity drugs and they are structurally related to amphetamine.20) It is known that phentermine does not release dopamine at a clinically significant quantity compared with amphetamine,5) but it is not possible to conclude that phentermine has no effect on dopamine.18) Likewise, a previous report emphasized that phentermine could elevate dopamine.13) Most cases associated with amphetamine analogues like phentermine did not show associative loosening or social withdrawal symptoms.13) In addiction, the report suggested the difference between psychosis induced by amphetamine analogues and schizophrenia is the absence of marked negative symptoms.13) Main positive symptoms of phentermine induced psychosis included persecutory delusion and auditory hallucination. Like previous report, our case did not show any significant negative symptoms but showed overt positive symptoms including persecutory delusion and auditory hallucination.
No studies have yet investigated longer-term psychosis related to phentermine although these symptoms can appear repeatedly and cause significant social impairment especially in young adults. Therefore, researches about chronicity or repetition of phentermine induced psychosis are needed in the near future. In addition, understanding who has a higher risk of developing psychotic symptoms could prevent physicians from letting these high-risk people to take phentermine. Thus, future studies should also focus on investigating individuals’ susceptibility of developing overt psychosis with phentermine administration. More importantly, the government has implemented a strict regulation to prevent patients from overdosing hypnotics, such as zolpidem and triazolam.26) The Korean government is also concerned about benzodiazepine abuse, but no regulation is implemented for phentermine despite the fact that it can cause severe psychopathologies (psychotic symptoms). This study suggests that, just like black box warning of selective serotonin reuptake inhibitor for suicide, there should be a precautious measure for physicians who plan to give phentermine to patients. Before prescribing phentermine, physicians should investigate patient’s history of psychiatric illness including psychotic disorder. In addition, precautious measurements are needed so that physicians would not overlook patient’s psychotic symptoms even if they are mild in severity. Moreover, patients who are prescribed phentermine need an education about psychiatric side effects.
Acknowledgments
This study was supported by Research Fund of Seoul St. Mary’s Hospital, The Catholic University of Korea (ZC16FISI0072). The authors have no conflict of interests.
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