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    Hyponatremia with olanzapine - A suspected association
    
                
    2017-11-29 03:44:40AnkurSACHDEVAMonaCHOUDHARY
    
                
    上海精神醫(yī)學(xué) 2017年3期 
    關(guān)鍵詞:警覺性低鈉血癥奧氮
    
                    
    Ankur SACHDEVA*, Mona CHOUDHARY
    Hyponatremia with olanzapine - A suspected association
    Ankur SACHDEVA1*, Mona CHOUDHARY2
    Hyponatremia, Olanzapine, Antipsychotics, India
    1. Case history
    A 45-year-old married Hindu female, non-smoker, non hypertensive and non diabetic, was diagnosed with paranoid schizophrenia, for which she was maintaining well on tablet haloperidol 20 mg/day for the last 5 years. The total duration of illness was around 7 years,with a drug naive period of approximately 2 years.Around three months ago, the patient’s symptoms had become exaggerated as she had not taken her antipsychotic medication for approximately 8-10 days because she was out of town and did not have her medicines with her. Her complaints were sleep disturbance, referential and persecutory ideas with intermittent auditory hallucinations and episodes of irritability with aggressive behavior. The patient presented to the hospital after which haloperidol was started again at 10 mg/day, increased to 20 mg/day and maintained for the next month. However no significant improvement was reported this time using haloperidol.Olanzapine 5 mg/day was added and increased to 10 mg/day within 2 weeks. One month after adding Olanzapine, the patient developed symptoms of nausea, anorexia and weakness. However there were no episodes of vomiting or diarrhea. Also, there was no significant decrement in diet. The symptoms exacerbated over the next 2 weeks along with muscle cramps, unsteady gait and fluctuating orientation.
    The patient was admitted to emergency services for evaluation. Her physical examination revealed tachycardia (pulse - 118/min), low blood pressure (94/60 mm hg), dehydration, and disorientation to time. Her systemic examination was unremarkable. Her blood tests revealed low serum sodium of 120 mmol/l (135-150 mmol/l). The results of the remaining tests were within normal limits (including renal function tests,liver function tests, serum concentrations of potassium,blood sugar, total proteins and lipids). Treatment was started on the diagnosis of probable normovolemic hyponatremia as physical examination did not reveal any signs of fluid overload. The electrocardiography revealed only sinus tachycardia and plasma osmolarity was reported to be 288 mOsm/kg H2O (285–295 mOsm/kgH2O). She was started on 3% NaCl infusion over the initial few hours until achieving full consciousness followed by normal saline. Fluid restriction and oral salt supplement was advised. The patient recovered in 2 days with serum sodium levels of 140 mmol/l. However,the exact reason for hyponatremia could not be established even after detailed investigations (including thyroid function tests). Olanzapine continued to be administered, except for the day emergency treatment was given. Upon detailed assessment, the patient’s diet was found to be consistently good over these years,and even during the last 2 weeks. No specific diet/salt restriction was reported.
    A week later, the patient again had similar episode of hyponatremia (serum sodium of 116 mmol/l) while continuing on the antipsychotics. She had to be managed in the emergency room with similar procedures and protocols. With no evident organic cause for the hyponatremia, a literature search was carried out and Olanzapine was postulated as a potential agent. It was planned to stop Olanzapine and observe the patient, while continuing medical management for hyponatremia. Within 3 days of stopping Olanzapine, the patient improved and never had a recurrence of hyponatremia over the next 6 months follow up. She was maintained on haloperidol 20 mg/day and risperidone 4 mg/day thereafter. Naranjo algorithm[1]established a “probable” causal relation between the drug and adverse event, with a total score of 8 (suggestive of a probable relationship).
    2. Discussion
    Olanzapine is a commonly used atypical antipsychotic for patients with schizophrenia and other psychotic disorders. In the CATIE study (Clinical Antipsychotic Trials of Intervention Effectiveness), Olanzapine was found to have the lowest discontinuation rate, possibly due to fewer incidences of acute side effects.[2]Still, life threatening adverse effects such as hyponatremia may limit its safe and effective use. A systematic review of evidence for antipsychotic induced hyponatremia from 1974 to 2003, found more cases of hyponatremia with typical compared to atypical antipsychotics.[3]
    Hyponatremia is the commonest electrolyte imbalance encountered in medical emergencies.[4]It is characterized by a plasma sodium concentration less than 135 mEq/L[5]and manifests clinically with neurological and systemic symptoms such as nausea,vomiting, anorexia, headache, disorientation,confusion, irritability and lethargy.[6]Profound hyponatremia may manifest as severe mental status changes including confusion, delirium, seizure, coma,and death. The most common causes of hyponatremia are fluid loss and dehydration, congestive heart failure,liver and renal failure, and Syndrome of inappropriate anti-diuretic hormone.
    Hyponatremia as a potential adverse event from the use of antipsychotics has not been greatly researched. Only a few case reports/series are available.[7,8]Meulendijks and colleagues did a systematic review of evidence for antipsychotic induced hyponatremia from 1974 to 2003 and found that both typical (58 case reports) and atypical antipsychotics (10 case reports) were implicated in hyponatremia and the association was independent of age or gender or dose.[3]Many antipsychotics (both typical and atypical) like chlorpromazine, fluphenazine,haloperidol, trifluoperazine, amisulpride, olanzapine and risperidone have been implicated.[3,9]Hyponatremia is postulated to be caused by blockade of inhibitory effect of dopamine on release of anti-diuretic hormone(ADH) by antipsychotics.[10]Clozapine, because of its low affinity for D2 receptors, is less prone to causing hyponatremia and may improve associated polydipsia.However on the contrary, it has been demonstrated in rats that dopamine could have a stimulatory effect on ADH release.[11]Therefore, the exact mechanism of antipsychotic-induced hyponatremia is still unclear.
    In the index case, hyponatremia and olanzapine were temporally associated, still it is difficult to establish the exact offending medication. Haloperidol is also a known culprit that is described in some case reports. However, haloperidol alone did not produce hyponatremia nor did it in combination with risperidone suggesting that olanzapine may have a stronger causal relation with hyponatremia.Also, Naranjo algorithm established a “probable”causal relationship with olanzapine. Another possible mechanism is that olanzapine precipitated hyponatremia in a predisposed individual taking haloperidol, and the causality may be attributed to the combined effect of both olanzapine and haloperidol.
    Hyponatremia is a rare yet clinically important adverse reaction to treatment with psychotropic drugs.It is a potentially dangerous medical complication in psychiatric patients. Psychogenic polydipsia is an important differential diagnosis, as it is characterized by similar symptoms of polydipsia and polyuria.Also, psychogenic polydipsia is commonly found in psychiatric patients, more likely in schizophrenia.[12]Multiple other factors such as diet, salt intake, ageing comorbid conditions (smoking, diabetes) or concurrent medications may also play a role and should be considered.[13]There is a complete and rapid recovery of drug induced hyponatremia once the offending agent is discontinued, as happened with the index case,without any further recurrences. Clinicians need to be aware of this dangerous complication and exercise caution when prescribing psychotropic drugs.
    Funding statement
    No funding support was obtained for preparing this case report.
    Conflict of interest statement
    The authors declare that they have no conflict of interest related to this manuscript
    Informed consent
    The patient and his guardian signed an informed consent form and agreed to the publication of this case report.
    1. Naranjo CA, Busto U, Sellers EM, Sandor P, Ruiz I, Roberts EA, et al. A method for estimating the probability of adverse drug reactions. Clin Pharmacol Ther. 1981; 30: 239-245.doi: http://dx.doi.org/10.1038/clpt.1981.154
    2. Lieberman JA, Stroup TS, McEvoy JP, Swartz MS, Rosenheck RA, Perkins DO, et al. Effectiveness of antipsychotic drugs in patients with chronic schizophrenia. N Eng J Med.2005; 353: 1209-1223. doi: http://dx.doi.org/10.1056/NEJMoa051688
    3. Meulendijks D, Mannesse CK, Jansen PA, van Marum RJ, Egberts TC. Antipsychotic-induced hyponatremia: A systematic review of the published evidence. Drug Saf.2010; 33: 101-14. doi: http://dx.doi.org/10.2165/11319070-000000000-00000
    4.Upadhyay A, Jaber BL, Madias NE. Incidence and prevalence of hyponatremia. Am J Med. 2006; 119(7 Suppl 1): S30–S35.doi: http://dx.doi.org/10.1016/j.amjmed.2006.05.005
    5. Biswas M, Davies JS. Hyponatraemia in clinical practice.Postgrad Med J. 2007; 83: 373–378. doi: http://dx.doi.org/10.1136/pgmj.2006.056515
    6.Sterns RH, Silver S, Kleinschmidt-DeMasters BK, Rojiani AM.Current perspectives in the management of hyponatremia:prevention of CPM. Expert Rev Neurother. 2007; 7: 1791–1797. doi: http://dx.doi.org/10.1586/14737175.7.12.1791
    7. Bakhla AK, Guria RT, Kumar A. A suspected case of olanzapine induced hyponatremia. Indian J Pharmacol.2014; 46(4): 441-442. doi: http://dx.doi.org/10.4103/0253-7613.135961
    8. Chiang CL, Lin YH, Hsieh MH. Olanzapine-induced hyponatremia in a patient with autism. J Child Adolesc Psychopharmacol. 2013; 23: 699-700. doi: http://dx.doi.org/10.1089/cap.2013.0055
    9. Collins A, Anderson J. SIADH induced by two atypical antipsychotics. Int J Geriatr Psychiatry. 2000; 15:282-283. doi: http://dx.doi.org/10.1002/(SICI)1099-1166(200003)15:3<282::AID-GPS89>3.0.CO;2-4
    10. Yamaguchi K, Hama H, Adachi C. Inhibitory role of paraventricular dopaminergic mechanisms in hemorrhage induced vasopressin secretion in conscious rats. Brain Res.1990; 513: 335-338
    11. Yamaguchi K, Hama H. Facilitatory role of central dopamine in the osmotic release of vasopressin. Brain Res. 1989;481(2): 388-391. doi: http://dx.doi.org/10.1016/0006-8993(89)90820-2
    12. Dundas B, Harris M, Narasimhan M. Psychogenic polydipsia review: Etiology, differential and treatment. Curr Psychiatry Rep. 2007; 9(3): 236–241
    13. Siegler EL, Tamres D, Berlin JA, Allen-Taylor L, Strom BL. Risk factors for the development of hyponatremia in psychiatric inpatients. Arch Intern Med. 1995; 155(9): 953-957. doi:http://dx.doi.org/10.1001/archinte.1995.00430090099011
    低鈉血癥與奧氮平——可能的關(guān)聯(lián)
    Sachdeva A, Choudhary M
    低鈉血癥;奧氮平;抗精神病藥
    Summary: Hyponatremia is a rare, yet potentially life threatening complication of antipsychotics. Here,we report a case of a 45-year-old female diagnosed with schizophrenia who developed hyponatremia soon after addition of olanzapine to the existing treatment. This prompted us to evaluate the relationship between hyponatremia and olanzapine, as timely management is crucial. Naranjo algorithm established a “probable” causal relation between olanzapine and hyponatremia. Possible etiological reasons of this clinically significant and life threatening adverse event have been discussed. We report the case and the literature focusing on hyponatremia as a possible adverse event of olanzapine. Medical illnesses are often ignored or missed in patients with psychiatric disorders either due to patients’ inability to report complaints or non-serious attitude of physicians towards such patients. A high index of suspicion should be kept while dealing with this probable complication.
    [Shanghai Arch Psychiatry. 2017; 29(3): 177-179.
    http://dx.doi.org/10.11919/j.issn.1002-0829.216053]
    1Department of Psychiatry, ESIC Medical College and Hospital, NH-3, NIT, Faridabad, Haryana, India,121001
    2Department of Psychiatry and Drug De-addiction, Post Graduate Institute of Medical Education and Research, Dr Ram Manohar Lohia Hospital, Park Street, New Delhi, India,110001
    *correspondence: Dr. Ankur Sachdeva, Mailing address: Department of Psychiatry, Room Number 9, ESIC Medical College and Hospital, NH-3, NIT,Faridabad, Haryana, India. Postcode: 121001, E-mail: drankur.rml@gmail.com
    概述:低鈉血癥是一種罕見的具有潛在生命危險的抗精神病藥物治療的不良反應(yīng)。這里,我們報告一個病例,45歲女性精神分裂癥患者在奧氮平治療后不久出現(xiàn)低鈉血癥。為此我們評估了低鈉血癥和奧氮平治療之間的關(guān)系,因為及時的藥物監(jiān)測至關(guān)重要。根據(jù)Naranjo算法,在奧氮平和低鈉血癥之間的關(guān)聯(lián)性評價,可評價為“可能”。因此有必要探究低鈉血癥這一臨床上重大、危及生命的不良事件產(chǎn)生的可能原因。我們報告的病例聚焦于奧氮平治療引起的低鈉血癥的不良事件。由于精神疾病患者有時無法主訴或主訴不被重視,內(nèi)科疾病常常被忽視或錯過。在處理這種可能的不良反應(yīng)時,應(yīng)保持高度警覺性。
    Dr. Ankur Sachdeva obtained his MBBS degree from Vardhman Mahavir Medical College and Safdarjang Hospital, New Delhi in 2009 and an MD (Psychiatry) degree from the Post Graduate Institute of Medical Education and Research, at the Dr. Ram Manohar Lohia Hospital in 2013. He subsequently received the Diplomate of the National Board (D.N.B) in psychiatry in 2014. He is presently working as Assistant Professor (Psychiatry) in ESIC medical college, Faridabad, Haryana,India.
    

    
                        
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