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    Case report of refractory tardive dystonia induced by olanzapine

    2014-12-09 03:44:08ZhenxiaoSUNXiangliWANG
    上海精神醫(yī)學(xué) 2014年1期
    關(guān)鍵詞:奧氮遲發(fā)性戊酸

    Zhenxiao SUN*, Xiangli WANG

    ?Case Report?

    Case report of refractory tardive dystonia induced by olanzapine

    Zhenxiao SUN*, Xiangli WANG

    movement disorders/adverse effects, olanzapine, schizophrenia

    1. Case history

    A 22-year old male was admitted to our hospital in June 2013 with a 6-year history of paranoid beliefs and auditory hallucinations and a 2-year history of torticollis.Starting in 2007 the patient had trouble concentrating,developed odd behaviors and reported auditory hallucinations of others talking about him. He became paranoid and believed that people were talking behind his back. He was intensely nervous and frightened because he believed that someone was trying to frame him or kill him. The patient’s family believed he was possessed, so they initially sought help from witch doctors and tried other folk remedies. But his condition continued to worsen and his social functioning became severely impaired.

    He was first brought to the outpatient department of a local psychiatric hospital by family members in April 2010. At that time his physical exam was normal and he was conscious and fully orientated but he had disorganized speech and reported auditory hallucinations and persecutory and referential delusions. He was diagnosed with schizophrenia and treated with olanzapine 5 mg/d, which was increased to 10 mg/d one week later. His psychotic symptoms began to improve after two months of treatment. The dose of olanzapine was reduced to 5 mg/d in August 2010. He continued taking the olanzapine regularly (without any adjunctive medications), but in June 2011 he began to experience lip puckering, right-side torticollis, muscular pain, muscular spasms in the trunk and unstable gait.His family dismissed these symptoms as the result of intense physical labor so he continued to take olanzapine 5 mg/d regularly.

    The physical impairment from the torticollis, spasms in the trunk muscles and gait instability continued to increase so the family brought him back to the local psychiatric hospital in December 2012. At that time the olanzapine was discontinued and replaced with haloperidol (6 mg/d), trihexyphenidyl (4 mg/d), and sodium valproate (0.6 g/d). However, this change in medication did not resolve the dystonic symptoms so the patient was eventually brought to our hospital for assessment in June 2013.

    On admission the patient had torticollis to the right side, axial dystonia and an abnormal gait, but was otherwise healthy with no history of severe physical diseases or allergies. His aunt had a history of mental illness, but there was no family history of tardive dystonia. Physical examination showed stable vital signs(body temperature: 37.50C; pulse: 92/m; respiratory rate: 20/m; blood pressure: 110/70 mmHg), normal heart and lung functioning, soft abdomen, and palpable liver and spleen. Neurological examination showed no abnormal results in the cranial nerves, no muscle atrophy or weakness in the four limbs, and normal muscle tone and deep tendon reflexes. A MRI of the head revealed no abnormalities.

    He was diagnosed with tardive dystonia and schizophrenia. He was treated with clozapine (starting at 12.5 mg/d and gradually increasing to 150 mg/d),magnesium valproate (sustained release tablets, 0.5 g bid), Vitamin E (1 g bid), tiapride (0.1 g bid), and lorazepam (1 mg tid). Despite taking this regimen regularly for one month as an inpatient and for a further three months as an outpatient, the TDt symptoms did not improve.

    2. Discussion

    Since the introduction of the first antipsychotics, there have been reports about persistent dystonia associated with their use. This antipsychotic-induced dystonia is considered a subtype of tardive dyskinesia. The concept of ‘dystonia tarda’ (subsequently called ‘tardive dystonia’ [TDt]) was proposed for the first time in 1973 when Keegan and Rajput reported a female patient who developed torticollis and scoliosis after taking antipsychotic medications.[1]Currently, it is considered a condition with many clinical features that are different from tardive dykinesia that is extremely difficult to cure. The occurrence of TDt is 2.7 to 5.3% among individuals taking antipsychotic medications.[2]TDt can appear at any stage of treatment and any antipsychotic medication can cause TDt; the different frequency of reported TDt with different antipsychotics is probably due to the different rates of prescribing the various medications.[2]The young male patient reported here developed lip puckering, persistent torticollis, pain, axial dystonia and unstable gait after one year of treatment with olanzapine. His symptoms, disease history, family history and physical examination were in line with the current diagnostic criteria of TDt.[3]

    Olanzapine is an atypical antipsychotic that binds to 5-tryptamine 2A receptors more than dopamine receptors and affects the mesolimbic dopamine pathway more than the nigrostriatal dopamine pathway.[4]Reports of olanzapine-induced TDt are rare. Searches of the China Journal Full-text Database (CNKI) and the Wanfang Database using keywords ‘olanzapine’ and‘tardive dystonia’ identified no report about tardive dystonia induced by olanzapine. A similar search of Pubmed only identif i ed nine case reports of olanzapineinduced TDt: Aggarwal and colleagues[4]report on a 17-year-old female with schizophrenia who developed symptoms of TDt after 15 months of treatment with olanzapine; Charf i and colleagues[5]report on a 17-yearold female with schizophrenia who manifested TDt symptoms after nine months of treatment with olanzapine; Singh and colleagues[6]reported on a case of TDt after using a single 10 mg dose of olanzapine;Aggarwal and colleagues[7]report on a case of delayed Meige syndrome (a combination of blepharospasm and oromandibular dystonia) after long-term usage of olanzapine; and Praharaj and colleagues[8]report on a young male patient who developed delayed oculogyric crisis following the use of olanzapine.

    The pathological and physiological mechanism of olanzapine-induced TDt is not clear. Trugman and colleagues[9]considered the sensitization of the D1-mediated striatal output after repetitive stimulation of the D1 receptor by endogenous dopamine the fundamental mechanism of TDt. According to this theory, olanzapine may cause TDt by persistent inhibition of dopamine neurotransmitters leading to overly sensitive postsynaptic dopamine receptors.[10]

    When treating patients with antipsychotic-induced TDt the first step is to change the current antipsychotic to another atypical antipsychotic. Clozapine should be tried first[5]; quetiapine and aripiprazole can then be tried. If the dystonic symptoms are serious, high dose anticholinergic agents (such as trihexyphenidyl at doses of 20 mg/d or higher) should be considered[11](especially among young patients) because this would deplete the excess of presynaptic dopamine; but this approach should not be used if symptoms of tardive dyskinesia are also present because anticholinergic agents can worsen these symptoms. There has been a report of TDt successfully treated by tetrabenazine.[12]There are also reports about the effectiveness of benzodiazepines such as diazepam, clonazepam or lorazepam.[13]Bhattacharjee and colleagues reported a case of olanzapine-induced TDt effectively treated by carbamazepine.[14]For TDt with only localized or mild symptoms, botulinum toxin A can be considered. For severe refractory axial dystonia,continuous intrathecal baclofen injection is considered the treatment of last resort,[16]but there is only limited evidence of the clinical effectiveness of this treatment.There have also been several case reports on using electroconvulsive therapy[17]and transcranial magnetic stimulation[18]to treat TDt; however, the evidence supporting these treatments is limited.

    In the current case, the patient’s family members failed to recognize the importance of the dystonia symptoms, so it took 18 months before his dystonic symptoms were first evaluated by a medical professional. The initial treatment for the dystonia(changing olanzapine to haloperidol) at the local hospital was probably not helpful (haloperidol can induce myotonic dystrophy syndrome[19]). By the time the dystonia was seen at our hospital it had already persisted for two years. We treated the patient’s refractory tardive dystonia with clozapine, magnesium valproate, vitamin E, tiapride, and lorazepam, but four months of treatment did not result in any improvement in the symptoms. The patient remains severely disabled by these symptoms so further more aggressive measures will need to be attempted, but the long-term prognosis for the patient remains guarded.

    There is no guarantee that earlier recognition and treatment of the tardive dystonia in this patient or in other patients with antipsychotic-induced TDt would improve their eventual outcome. Most reports indicate that the TDt symptoms persist after patients stop taking antipsychotics.[20]Further research is needed to identify effective treatments for TDt. Nevertheless, the severe disability associated with this uncommon sideeffect makes it imperative that patients, their family members, and all clinicians who prescribe antipsychotic medications be well informed about this potential side effect and the need to urgently seek treatment when dystonic symptoms occur. Family education is particularly important in rural settings where the intervals between follow-up medical visits for medicated psychiatric patients can be several months. Clinicians who prescribe antipsychotic medication must carefully monitor extrapyramidal symptoms at every followup visit and keep up-to-date on the best methods for dealing with this severe adverse reaction.

    Acknowledgement

    The patient reported in this case report provided written informed consent for the publication of this report.

    Conflict of interest

    The authors report no conflict of interest related to this manuscript.

    1. Keegan DL, Rajput AH. Drug induced dystonia tarda:treatment with L-dopa. Dis Nerv Syst. 1973;34(3): 167-169

    2. Sun ZX, Yu XF. [Progress in studies on tardive dystonia induced by antipsychotic drugs].Yao Wu Bu Liang Fan Ying Za Zhi. 2012;14(1): 34-38. Chinese

    3. Yan WW. [Be on guard for the occurrence of tardive dyskinesia and tardive dystonia]. Shang Hai Jing Shen Yi Xue.2006;18(3): 186-189. Chinese

    4. Aggarwal A, Jiloha RC. Olanzapine induced tardive dystonia.Indian J Pharmacol. 2008;40(5): 237-238. doi: http://dx.doi.org/10.4103/0253-7613.44158

    5. CharfiF, Cohen D, Houeto JL, Soubrié C, Mazet P.Tardive dystonia induced by atypical neuroleptics:a case report with olanzapine. J Child Adolesc Psychopharmacol. 2004;14(1): 149-152. doi: http://dx.doi.org/10.1089/104454604773840607

    6. Singh GP, Kumar R, Bharti P. Tardive dystonia with olanzapine: a rare case report. Indian J Psychol Med. 2012;34(2): 187-189. doi: http://dx.doi.org/10.4103/0253-7176.101795

    7. Aggarwal A, Jain M, Khandelwal A, Jiloha RC. Tardive Meige’s syndrome associated with olanzapine. Ann Indian Acad Neurol. 2011;14(2): 133-134. doi: http://dx.doi.org/10.4103/0972-2327.82808

    8. Praharaj SK, Jana AK, Sarkar S, Sinha VK. Olanzapineinduced tardive oculogyric crisis. J Clin Psychopharmacol.2009;29(6): 604-606. doi: http://dx.doi.org/10.1097/JCP.0b013e3181c00b08

    9. Trugman JM, Leadbetter R, Zalis ME, Burgdorf RO, Wooten GF. Treatment of severe axial tardive dystonia with clozapine:case report and hypothesis. Mov Disord. 1994;9(4): 321-324. doi: http://dx.doi.org/10.1002/mds.870090411

    10. Van Harten PN, Kahn RS. Tardive dystonia. Schizophrenia Bull. 1999;25(4): 741-748

    11. Kiriakakis V, Bhatia KP, Quinn NP, Marsden CD. The natural history of tardive dystonia. A long-term follow-up study of 107 cases. Brain. 1998;121(11): 2053-2066. doi: http://dx.doi.org/10.1093/brain/121.11.2053

    12. Rauchverger B, Isakov V, Jabarin M. Olanzapine-induced tardive dystonia successfully treated by tetrabenazine. J Neuropsychiatry Clin Neurosci. 2007;19(4): 484-485. doi:http://dx.doi.org/10.1176/appi.neuropsych.19.4.484-a

    13. Blake LM, Marks RC, Nierman P, Luchins DT. Clozapine and clonazepam in tardive dystonia. J Clin Psychopharmacol.1991;11(4): 268-269

    14. Bhattacharjee S, Tiwari M, Dutt A, Kumar H. Olanzapineinduced task specific tardive dystonia and its response to carbamazepine: a case report. Neurol India. 2012;60(6):649-650. doi: http://dx.doi.org/10.4103/0028-3886.105207

    15. Tarsy D, Kaufman D, Sethi KD, Rivner MH, Molho E, Factor S.An open-label study of botulinum toxin A for treatment of tardive dystonia. Clin Neuropharmacol. 1997;20(1): 90-93.doi: http://dx.doi.org/10.1097/00002826-199702000-00012 16. Dressler D, Oeljeschl?ger RO, Rüther E. Severe tardive dystonia: treatment with continuous intrathecal baclofen administration. Mov Disord. 1997;12(4): 585-587. doi:http://dx.doi.org/10.1002/mds.870120416

    17. Sienaert P, Peuskens J. Remission of tardive dystonia(blepharospasm) after electroconvulsive therapy in a patient with treatment-refractory schizophrenia. J ECT. 2005;21(2):132-134

    18. Andrews C, Aviles-Olmos L, Hariz M, Foltynie T. Which patients with dystonia benef i t from deep brain stimulation?A metaregression of individual patient outcomes. J Neurol Neurosurg Psychiatry. 2010;81(12): 1383-1389. doi: http://dx.doi.org/10.1136/jnnp.2010.207993

    19. Bhidayasiri R, Fahn S, Weiner WJ, Gronseth GS, Sullivan KL, Zesiewicz TA. Evidence-based guideline: treatment of tardive syndromes: report of the Guideline Development Subcommittee of the American Academy of Neurology.Neurology. 2013;81(5): 463- 469. doi: http://dx.doi.org/10.1212/WNL.0b013e31829d86b6

    20. Sun ZX, Yu XF. [Clinical characteristics and follow-up study of 12 patients with tardive dystonia caused by antipsychotics].Zhong Guo Zhi Ye Yao Shi. 2012;9(4): 3-6

    奧氮平所致難治性遲發(fā)性肌張力障礙1例

    孫振曉, 王相立

    遲發(fā)性肌張力障礙是長期使用抗精神病藥物所致的一系列錐體外系癥狀,主要特征包括骨骼肌肉(隨意?。┳灾鬟\(yùn)動(dòng)困難和隨后的軀體變形。遲發(fā)性肌張力障礙在服用奧氮平患者中罕見,但本文報(bào)道中奧氮平正是這名22歲男性精神分裂癥患者的促發(fā)抗精神病藥物,他堅(jiān)持服用標(biāo)準(zhǔn)劑量的奧氮平大約1年后出現(xiàn)撅嘴、持續(xù)不自主斜頸、肌肉疼痛、軸向肌張力障礙和步態(tài)不穩(wěn)的癥狀。停用奧氮平后,他的癥狀沒有緩解。氯氮平合并丙戊酸鎂、維生素E、硫必利和勞拉西泮治療四個(gè)月也沒有讓肌張力障礙得到任何改善。

    運(yùn)動(dòng)障礙/不良反應(yīng),奧氮平,精神分裂癥

    Tardive dystonia (TDt), a cluster of extrapyramidal symptoms that are caused by long-term use of antipsychotic medication, is characterized by difficulty in autonomic movements of skeletal (voluntary)muscles and consequent deformations of the body. TDt is rarely seen among patients taking olanzapine, but olanzapine was the precipitating antipsychotic medication in this 22-year old male patient with schizophrenia who developed lip puckering, persistent involuntary torticollis, muscular pain, axial dystonia and unstable gait after taking a standard dose of olanzapine regularly for about one year. His symptoms did not resolve after his olanzapine was stopped. Four months of treatment with clozapine combined with magnesium valproate,vitamin E, tiapride, and lorazepam did not lead to any improvement in the dystonia.

    http://dx.doi.org/10.3969/j.issn.1002-0829.2014.01.008

    Linyi Mental Health Center, Linyi, Shandong Province, China

    *correspondence: szx.ywk@163.com

    A full-text Chinese translation will be available at www.saponline.org on April 15, 2014.

    (received: 2013-11-28; accepted: 2013-12-30)

    Dr. Zhenxiao Sun graduated from Heze Medical Technical College in 1989 and from Jining Medical College with a bachelor’s degree in clinical medicine in 2007. He has been working in Shandong Province Linyi Mental Health Center since 1989. He is currently the vice-president of the hospital and a senior psychiatrist. His main research interest is clinical psychopharmacology.

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