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To the Editor: Restless legs syndrome (RLS) is a common neurological movement disorder characterized by an unpleasant sensation in and the urge to move the legs, affecting approximately 10% of adults, but it is often underdiagnosed or misdiagnosed.1,2
There have been very few reports of RLS secondary to the use of antipsychotics like olanzapine,3,4 quetiapine,5 and clozapine.6 We report a case of clozapine-induced RLS, which improved with add-on aripiprazole.

Case Report

“Ms. M,” a 34-year-old woman with a 12-year history of treatment-resistant paranoid schizophrenia, having auditory hallucinations and multiple delusions, had poor response to adequate trials of haloperidol, risperidone, and injection fluphenazine. Because of treatment nonresponse, she was started on clozapine, which was increased to 200 mg. Within a week of starting clozapine, she complained of discomfort in the form of pain in both legs mainly, but also with a lesser intensity in both arms, which would begin within 1 hour of taking clozapine at night. The symptoms were relieved by movement of legs by stretching her muscles by massaging them throughout the night. This would last for 3–4 hours, and she developed initial insomnia. Her neurological examination was within normal limits, with no evidence of peripheral neuropathy. The pain continued to persist even when clozapine was decreased to 100 mg. As the symptoms began after antipsychotic use, akathisia was initially suspected, and promethazine 25 mg was started, with no significant improvement. Hemogram revealed hemoglobin 13 g/dl, normocytic normochromic blood picture with normal total and differential counts. Renal, liver, and thyroid function tests, blood glucose, electroencephalogram, and brain imaging (computed tomography) were within normal limits. Akathisia was ruled out because of the presence mainly of discomfort without any subjective restlessness relieved by stretching, nocturnal nature of symptoms, and accompanying sleep disturbance. She was clinically diagnosed to have restless leg syndrome as per the International Restless Legs Syndrome Study Group Rating Scale (IRLS), having an IRLS score of 27, which indicates severe RLS.7 Polysomnography and serum ferritin could not be done for this patient. She was started on diazepam 5 mg. Clozapine was increased to 200 mg because of the severity of psychotic symptoms. She was discharged on clozapine 200 mg and diazepam 5 mg. No improvement in RLS was noted with diazepam 5 mg. She continued to have RLS while being on clozapine for nearly 6 months. Discontinuation of clozapine could not be considered; as the patient was nonresponsive to other treatment; but further increase in clozapine was deferred because of persisting RLS. She was again admitted because of severity of symptoms. At admission, Brief Psychiatric Rating Scale score was 45. She was given aripiprazole 10 mg as an augmenting agent to clozapine. Within 2 days of adding aripiprazole 10 mg, her RLS subsided, with an IRLS score of 4. There was no recurrence of RLS even when clozapine was increased to 300 mg while aripiprazole 10 mg continued. She continues to maintain remission of RLS for 8 months on aripiprazole 10 mg, with an IRLS score of 0. Her current BPRS score is 18 on clozapine 300 mg, with continuing improvement in functioning.

Discussion

RLS may be a primary condition, or may be secondary to iron deficiency, pregnancy, renal failure, medication side effects, or spinal cord injury. The improvement of RLS symptoms with dopaminergic therapy and reversal of the beneficial effects of dopamine agonists by antagonists supports the role of dopamine in RLS.8
There have been reports of antipsychotic-induced RLS with olanzapine,3,4 quetiapine,5 and clozapine. Symptoms of RLS secondary to antipsychotic use has to be initially differentiated from akathisia, in which the desire to move is not necessarily associated with discomfort in the legs; subjective restlessness is very high; and symptoms are not worse at night. In most of the earlier reports of antipsychotic-induced RLS, either antipsychotic dosage was reduced or antipsychotic was stopped and changed. In others, approved drugs for RLS, like ropinirole or propoxyphene was used. In this case, the use of the Naranjo et al. Adverse Drug Reaction Probability Scale9 (score: 5) indicated that the adverse effect was probably related to clozapine. Per our knowledge, this is the first case of antipsychotic-induced RLS, in this case clozapine, that was treated by aripiprazole.
This patient had none of the common causes of RLS and the temporal correlation with clozapine intake was considered as an indicator of clozapine being the offending agent.
Aripiprazole has a unique mechanism of weak partial agonism at D2-like dopamine receptors, with 95% receptor occupancy at clinical doses in PET studies.10 This unique partial agonism of dopaminergic system also could explain its role in alleviating RLS that is similar to other approved drugs for RLS such as dopamine agonists like ropinirole and pramipexole. Aripiprazole also had the added benefit of having a synergistic effect with clozapine,11 which enabled in improvement in the psychotic symptoms and enabled further increase in clozapine dosage, as well. Therefore, in antipsychotic-induced RLS, aripiprazole could be considered, as it would also have an added antipsychotic effect and, in a case like this, wherein the antipsychotic could not be stopped, as the patient was a nonresponder, and the psychotic symptoms were very severe.

References

1.
Hening W, Walters AS, Allen RP, et al.: Impact, diagnosis, and treatment of restless legs syndrome (RLS) in a primary care population: the REST (RLS epidemiology, symptoms, and treatment) primary care study. Sleep Med 2004; 5:237–246
2.
Bjorvatn B, Leissner L, Ulfberg J, et al.: Prevalence, severity, and risk factors of restless legs syndrome in the general adult population in two Scandinavian countries. Sleep Med 2005; 6:307–312
3.
Khalid I, Rana L, Khalid TJ, et al.: Refractory restless legs syndrome likely caused by olanzapine. J Clin Sleep Med 2009; 5:68–69
4.
Kang SG, Lee HJ, Kim L: Restless legs syndrome and periodic limb movements during sleep probably associated with olanzapine. J Psychopharmacol 2009; 23:597–601
5.
Pinninti NR, Mago R, Townsend J, et al.: Periodic restless legs syndrome associated with quetiapine use: a case report. J Clin Psychopharmacol 2005; 25:617–618
6.
Duggal HS, Mendhekar DN: Clozapine-associated restless legs syndrome. J Clin Psychopharmacol 2007; 27:89–90
7.
Walters AS, LeBrocq C, Dhar A, et al.: International Restless Legs Syndrome Study Group: Validation of the International Restless Legs Syndrome Study Group rating scale for restless legs syndrome. Sleep Med 2003; 4:121–132
8.
Chahine LM, Chemali ZN: Restless legs syndrome: a review. CNS Spectr 2006; 11:511–520
9.
Naranjo CA, Busto U, Sellers EM, et al.: A method for estimating the probability of adverse drug reactions. Clin Pharmacol Ther 1981; 30:239–245
10.
Grunder G, Carlsson A, Wong DF: Mechanism of new antipsychotic medications: occupancy is not just antagonism. Arch Gen Psychiatry 2003; 60:974–977
11.
Muscatello MR, Bruno A, Pandolfo G, et al.: Effect of aripiprazole augmentation of clozapine in schizophrenia: a double-blind, placebo-controlled study. Schizophr Res 2011; 127:93–99

Information & Authors

Information

Published In

Go to The Journal of Neuropsychiatry and Clinical Neurosciences
Go to The Journal of Neuropsychiatry and Clinical Neurosciences
The Journal of Neuropsychiatry and Clinical Neurosciences
Pages: E62 - E63
PubMed: 23686071

History

Published online: 1 April 2013
Published in print: Spring 2013

Authors

Details

Dhanya Raveendranathan, M.D.
Department of Psychiatry National Institute of Mental Health And Neurosciences (NIMHANS), Bangalore, India
Lakshmi Shiva, M.B.B.S.
Department of Psychiatry National Institute of Mental Health And Neurosciences (NIMHANS), Bangalore, India
Ganesan Venkatasubramanian, M.D.
Department of Psychiatry National Institute of Mental Health And Neurosciences (NIMHANS), Bangalore, India
Mukund G. Rao, M.D.
Department of Psychiatry National Institute of Mental Health And Neurosciences (NIMHANS), Bangalore, India
Shivarama Varambally, M.D.
Department of Psychiatry National Institute of Mental Health And Neurosciences (NIMHANS), Bangalore, India
Bangalore N. Gangadhar, M.D.
Department of Psychiatry National Institute of Mental Health And Neurosciences (NIMHANS), Bangalore, India

Notes

Correspondence: Dr. Raveendranathan; Dept. of Psychiatry, National Institute of Mental Health And Neurosciences, Bangalore, India; e-mail: [email protected]

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