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AUTHOR AND EDITOR INFORMATION

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Author: Mary C Mancini, MD, PhD, Director of Cardiothoracic Transplantation, Professor, Department of Surgery, Louisiana State University Health Sciences Center

Mary C Mancini is a member of the following medical societies: American Heart Association, American Medical Association, American Thoracic Society, Association for Academic Surgery, Association for Surgical Education, International College of Surgeons, International Society for Heart and Lung Transplantation, New York Academy of Sciences, Phi Beta Kappa, and Southern Thoracic Surgical Association

Coauthor(s): Girish G Deshpande, MD, MBBS, FAAP, Assistant Professor, Department of Pediatrics, Division of Critical Care Medicine, Children's Hospital of Illinois at OSF St Francis Medical Center

Editors: G Patricia Cantwell, MD, Associate Clinical Professor, Department of Pediatrics, University of Miami; Director of Pediatric Critical Care Medicine, Miller School of Medicine, Jackson Children's Hospital; Mary L Windle, PharmD, Adjunct Assistant Professor, University of Nebraska Medical Center College of Pharmacy, Pharmacy Editor, eMedicine.com, Inc; Barry J Evans, MD, Assistant Professor of Pediatrics, Temple University Medical School; Director of Pediatric Critical Care and Pulmonology, Associate Chair for Pediatric Education, Temple University Children's Medical Center; Mary E Cataletto, MD, Associate Director, Division of Pediatric Pulmonology, Winthrop University Hospital; Associate Professor, Department of Clinical Pediatrics, State University of New York at Stony Brook; Maureen Strafford, MD, Arnold P Gold Foundation Associate Professor, Departments of Anesthesiology and Pediatrics, Tufts University and Tufts-New England Medical Center

Author and Editor Disclosure

Synonyms and related keywords: neuroleptic malignant syndrome, NMS, neuroleptics, antidopaminergic activity, serotonin

INTRODUCTION

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Background

Neuroleptic malignant syndrome (NMS), first described in 1963 by Delay et al in the French psychiatric literature, is a rare but potentially lethal complication of treatment with potent neuroleptics.

Neuroleptic drugs (ie, antipsychotic drugs, antischizophrenic drugs) are primarily used to treat schizophrenia and other psychotic states. Traditional drugs have action through inhibition of dopaminergic receptors, while the newer agents work by causing blockade of serotonin receptors.

NMS often occurs as treatment begins, when physicians progressively increase doses of neuroleptics. No clear relationship has been established between neuroleptic dosage and risk of developing NMS. A drug's potential for inducing NMS seems to parallel its antidopaminergic activity.

Pathophysiology

NMS pathophysiology is largely speculative. Neuroleptic drugs block dopaminergic receptors, creating a functional dopamine-deficiency state. Dopaminergic receptor blockade in the substantia nigra causes muscle rigidity and alters thermoregulation in the hypothalamus. Increased heat production from muscle rigidity causes fever, impaired heat dissipation (by reducing cutaneous vasodilatation or by sweating), and possibly a higher core temperature set point in the hypothalamus.

MM isoenzyme of creatine kinase increases. Muscle biopsy demonstrates morphologic and histoenzymologic abnormalities in muscle fibers.

Frequency

International

Incidence varies because of differing diagnostic criteria, patient characteristics, and available information. Reported incidence of NMS in neuroleptic-treated patients ranges from 0.1-5.5%.

NMS onset ranges from 1-44 days following administration of neuroleptic drug; mean onset is 10 days. Lazarus et al reported NMS occurring in 67% of patients within 1 week and 96% of patients within 30 days following administration of neuroleptics.

Mortality/Morbidity

Once reported to be 20-30%, the mortality rate is now estimated at 5-11.6%. Mortality is caused by one or more complications (eg, respiratory failure, cardiovascular collapse, renal failure, arrhythmias, thromboembolism). Renal failure is associated with a 50% mortality rate.

No consistent long-term physical, neurological, cognitive, or laboratory sequelae have been attributed to NMS alone, although sequelae may result from such secondary complications as prolonged hypoxia or ischemic encephalopathy. Researchers have noted sporadic cases of prolonged rigidity and long-term neuropsychological deficits.

Sex

The male-to-female ratio is 2:1.

Age

NMS occurs in people of all age groups, with a reported mean age of 40 years.


CLINICAL

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History

  • Symptoms
    • Neuroleptics either recently started or dosage recently increased
    • NMS usually evolves over 24-72 hours.
    • Hyperthermia (temperature >38°C)
    • Altered mental status
    • Rigidity and other extrapyramidal syndrome (EPS) symptoms
    • Autonomic dysfunction (eg, urinary incontinence, diaphoresis, sialorrhea)
    • Dyspnea, dysphagia

Physical

  • General examination
    • Hyperthermia
    • Tachycardia
    • Tachypnea, respiratory distress (31% of cases)
    • Hypotension or hypertension
    • Hypoxemia (low pulse oximeter reading)
    • Dehydration (secondary to hyperpyrexia and inadequate oral intake)
  • Neuromuscular examination
    • Altered mental status (status ranging from drowsiness and confusion to coma)
    • Muscular rigidity (usually lead-pipe type)
    • Autonomic dysfunction (eg, dysrhythmias, urinary incontinence, diaphoresis, sialorrhea, tachycardia, hypotension, hypertension)
    • Other EPS

Causes

  • Most common agents
    • Butyrophenones
    • Haloperidol
    • Phenothiazines
    • Thioxanthenes
    • Long-acting neuroleptics (benzamines)
    • Several other agents that reportedly have caused NMS - Tricyclic antidepressants, monoamine oxidase inhibitors (MAOIs), anticonvulsants, lithium, and dopamine antagonists (eg, metoclopramide, sulpiride)
  • Agent risk factors
    • Rapid initiation of antipsychotic therapy
    • Use of high-potency drugs (drug's potential for inducing NMS seems to parallel its antidopaminergic activity)
    • Depot preparations
  • Host risk factors
    • Age - People of all age groups affected (reported mean age is 40 years)
    • Sex - More common in men (2:1 ratio)
    • Concomitant illnesses
      • Organic brain disease or alcoholism
      • Dehydration, nutritional deficits
      • Affective disorder
      • Severe patient agitation or catatonia
      • History of NMS
      • Simultaneous use of predisposing drugs (eg, lithium, anticholinergic agents)
  • Environmental risk factors: Environmental risk factors may include seasonality. Some investigators report higher incidence of NMS in summer in connection with heat stroke; other investigators have reported no seasonal clustering.
  • Caveats
    • Higher incidence of NMS with parenteral administration of neuroleptics was noted in one study.
    • Coadministration of anti-Parkinson drugs and neuroleptics effectively prevents NMS, according to one investigator; however, another investigator found no such benefit. Withdrawal of parkinsonian medication is reported to be one etiological factor for NMS.
    • Not all patients have recurrent NMS, even if the same neuroleptic is administered in the same dose after recovery from NMS.


DIFFERENTIALS

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Bacteremia
Head Trauma
Hyperthyroidism
Meningitis, Aseptic
Meningitis, Bacterial
Multiple Endocrine Neoplasia
Pheochromocytoma
Schizophrenia and Other Psychoses
Substance Abuse: Cocaine
Systemic Lupus Erythematosus
Tetanus
Thyroid Storm
Toxicity, Monoamine Oxidase Inhibitor
Toxicity, Selective Serotonin Reuptake Inhibitor

Other Problems to be Considered

NMS is a diagnosis of exclusion; the following disorders create similar symptomatology:

Primary CNS disorders

Meningoencephalitis
Stroke
Trauma
Tumors
Major psychosis (eg, lethal catatonia)

Systemic disorders

Infections (eg, tetanus)
Metabolic conditions
Endocrinopathies (eg, thyrotoxicosis, pheochromocytoma)
Autoimmune diseases (eg, systemic lupus erythematosus)
Sepsis

Miscellaneous

Heat stroke
Strychnine poisoning
Central anticholinergic syndrome
Sympathomimetic intoxication
Serotonin syndrome
MAOI overdose
Lithium overdose
Alcohol or sedative-hypnotic withdrawal
Malignant hyperthermia


WORKUP

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Lab Studies

  • No laboratory test result is diagnostic for NMS.
  • Evidence of increased muscular activity includes the following:
    • Elevated creatinine kinase (50-100% of cases)
    • Metabolic acidosis
    • Increased transaminases
    • Myoglobinuria
  • Complete blood cell count showing leukocytosis (70-98% of cases)
  • Electrolyte levels indicating hyperkalemia, metabolic acidosis
  • Renal function tests indicating prerenal (dehydration) and renal (myoglobinuria) failure
  • Coagulation studies, such as platelet count, prothrombin time (PT), and activated partial thromboplastin time (aPTT), if thromboembolic phenomenon or diffuse intravascular coagulation (DIC) is suspected
  • Cultures from various sites to look for infections
  • Cerebrospinal fluid (CSF) analysis to rule out meningitic or encephalitic process

Imaging Studies

  • Imaging studies (eg, CT scanning, MRI) of the brain may be performed to rule out other conditions such as intracranial hemorrhage (ICH) or trauma. They per se do not yield any diagnostic information for NMS.
  • Chest radiography for suspected aspiration pneumonia

Histologic Findings

NMS has an associated increase of MM isoenzyme of creatine kinase. Muscle biopsy demonstrates morphological and histoenzymological abnormalities in muscle fibers. These findings are nonspecific and are not diagnostic of NMS.


TREATMENT

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Medical Care

NMS is a life-threatening medical emergency that requires monitoring and management in an ICU. Tailor intervention levels to the severity of illness.

  • Terminate the dopamine antagonist by withdrawing neuroleptic and NMS-potentiating drugs (eg, anticholinergics, lithium).
  • Supportive measures include the following:
    • Reduce body temperature using antipyretics, evaporative cooling, ice packs, and cooled IV fluids.
    • Treat suspected or secondary infections with empiric antibiotics.
    • Consider prophylactic intubation for patients with excessive salivation, swallowing dysfunction, coma, hypoxemia, acidosis, and severe rigidity with hyperthermia.
    • Maintain pulmonary, cardiovascular, and renal functions by monitoring and managing such complications as respiratory failure, renal failure, DIC, and arrhythmias.
    • Sedate the patient.
  • Specific measures include the following:
    • A goal is rapid peripheral muscle relaxation. Rapid control of rigidity averts hyperthermia, rhabdomyolysis, renal failure, pneumonia, respiratory failure, DIC, and cardiovascular collapse.
    • Considering all the disadvantages of dantrolene (vide infra), using nondepolarizing neuromuscular blocking agents (eg, pancuronium, other newer agents) is reasonable, along with such sedatives as benzodiazepines, to achieve rapid, predictable, and effective control of rigidity and hyperthermia.
    • Dantrolene sodium directly relaxes muscles by inhibiting calcium release from the sarcoplasmic reticulum. Its disadvantages include the following: the mean response time is 1.7 days; rigidity and temperature reduction takes longer, effects are erratic, and effects are often incomplete; and dantrolene is a potentially hepatotoxic agent. Because of rigidity relieving action, it may offer another therapeutic modality for treatment of NMS.
    • Bromocriptine is a dopamine agonist that overcomes neuroleptic-induced dopaminergic blockade. It has also been used in combination with dantrolene.
    • Other agents that have been tried include amantadine, which enhances presynaptic release of dopamine, and levodopa/carbidopa, which increase presynaptic dopamine stores.
    • Antimuscarinic agents are not recommended because they are not only ineffective but also may worsen hyperthermia.
  • Consider electroconvulsive therapy (ECT). In 1987, Addonizio and Susman recommended ECT for persistently psychotic and agitated patients in whom distinguishing between NMS and lethal catatonia is difficult and in patients who run the risk of NMS recurring when neuroleptics are restarted.

Consultations

Consultation with a psychiatrist may be prudent as the patient is stabilized in the ICU and for further follow-up care after the patient is discharged from the ICU.


MEDICATION

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Drug Category: Skeletal muscle relaxants, nonparalytic

This agent is a direct muscle relaxant to control rigidity.

Drug NameDantrolene sodium (Dantrium)
DescriptionInterferes with release of calcium from sarcoplasmic reticulum, thus directly inhibiting muscle contraction. Also prevents or reduces increase in myoplasmic calcium ion concentration that activates acute catabolic process associated with malignant hyperthermia. Available as sodium salt in 25-, 50-, and 100-mg caps and in 20-mg powder for injection.
Adult DoseSpasticity: 25 mg/d PO initially, gradually increase to tid/qid; then increase dose by 25 mg q4-7d; not to exceed 100 mg 2-4 times/d or 400 mg/d
Hyperthermia:
Preoperative prophylaxis: 4-8 mg/kg/d PO divided qid administered 1-2 d before surgery for patients at risk; to prevent recurrence, administer last dose 3-4 h before scheduled surgery; alternatively, 2.5 mg/kg IV 1.25 h before surgery and infused over 1 h; additional doses may be needed during surgery, especially if prolonged
Crisis: 1 mg/kg IV, may repeat prn; not to exceed a cumulative dose of 10 mg/kg; if physiologic and metabolic abnormalities reappear, repeat regimen
Postcrisis follow-up: 4-8 mg/kg/d PO divided qid for 1-3 d; administer IV when PO therapy is not practical; individualize dosage beginning with 1 mg/kg IV or more as clinical situation dictates
Pediatric DoseSpasticity: 0.5 mg/kg PO bid initially, increase frequency to tid/qid at 4- to 7-d intervals; then increase dose by 0.5 mg/kg; not to exceed 3 mg/kg 2-4 times/d up to 400 mg/d
Hyperthermia: Administer as in adults
ContraindicationsDocumented hypersensitivity; active hepatic disease (eg, hepatitis, cirrhosis)
InteractionsUse with verapamil may result in hyperkalemia and myocardial depression; concomitant use of estrogen increases risk of hepatotoxicity; CNS depression is exaggerated when used with CNS depressants; incompatible when mixed with dextrose, saline, or bacteriostatic water solutions
PregnancyC - Safety for use during pregnancy has not been established.
PrecautionsCaution with impaired cardiac or pulmonary function or history of previous liver disease; may cause hepatotoxicity (more common in females or patients >35 y), onset of overt hepatitis typically 3-12 mo after treatment initiation; monitor baseline and periodic liver function; adverse reactions include hepatitis, drowsiness, seizures, dizziness, lightheadedness, confusion, headaches, pleural effusion with pericarditis, tachycardia, hematuria, diarrhea, nausea, vomiting, GI bleeding, severe constipation, dysphagia, rash, photosensitization, acnelike rash, pruritus, urticaria, and abnormal hair growth; avoid alcohol and unnecessary exposure to sunlight; causes drowsiness; may impair ability to perform hazardous functions requiring mental alertness or physical coordination; protect IV from light; use reconstituted injection within 6 h; precipitant forms when IV placed in glass containers

Drug Category: Dopamine agonists

For a dopamine agonist to offer clinical benefit, it must stimulate D2 receptors. D2 receptor blockade might cause NMS by removing tonic inhibition from the sympathetic nervous system or more directly by neuroleptic agents (eg, phenothiazines).

Drug NameBromocriptine (Parlodel)
DescriptionIs an ergot alkaloid with dopamine receptor agonist action.
Adult Dose10 mg PO tid initially; if no improvement in 24 h, may increase dose; not to exceed 20 mg PO qid
Pediatric DoseLimited data exist; 1.25 mg PO q12h initially, may gradually increase dose prn; not to exceed 20 mg/d
ContraindicationsDocumented hypersensitivity; ischemic heart disease; peripheral vascular disorders
InteractionsToxicity may increase with ergot alkaloids; amitriptyline, butyrophenones, imipramine, methyldopa, phenothiazines, and reserpine may decrease bromocriptine effects
PregnancyB - Usually safe but benefits must outweigh the risks.
PrecautionsMay worsen condition of patient with psychiatric illness, peptic ulcer disease, or preexisting peripheral vascular disease; may result in cardiac decompensation in patients with history of myocardial infarction; adverse reactions include orthostatic hypotension, hallucinations, confusion, delirium, nausea, and vomiting

Drug NameAmantadine (Symmetrel)
DescriptionHas been tried in NMS because it increases synaptic dopamine activity. As an antiviral, actions include inhibition of influenza A virus uncoating, prevention of virus penetration into host, and inhibition of M2 protein in the assembly of progeny virions. Exhibits antiparkinsonian activity by blocking reuptake of dopamine into presynaptic neurons and by causing direct stimulation of postsynaptic receptors.
Adult DoseLimited data exist; several case reports describe using 100 mg PO bid
Pediatric DoseNot established; 5 mg/kg/d PO qd or divided bid has been used for influenza A prophylaxis; not to exceed 150 mg/d (age 1-9 y) or 200 mg/d (age >10 y)
ContraindicationsDocumented hypersensitivity
InteractionsDrugs with anticholinergic or CNS stimulant activity increase amantadine toxicity; the concurrent administration of hydrochlorothiazide plus triamterene with amantadine may increase plasma concentrations of amantadine
PregnancyC - Safety for use during pregnancy has not been established.
PrecautionsCaution with liver disease, epilepsy, history of recurrent eczematoid dermatitis, or uncontrolled psychosis; may increase seizure activity or EEG disturbances with preexisting seizure disorders; decrease dosage with renal impairment and with active seizure disorders; adverse reactions include orthostatic hypotension, edema, dizziness, confusion, insomnia, difficulty in concentration, restlessness, hallucinations, seizures, livido reticularis, nausea, vomiting, xerostomia, and urinary retention; avoid alcohol; may cause drowsiness; may impair ability to perform activities requiring mental alertness or coordination; do not abruptly discontinue therapy because may precipitate a parkinsonian crisis

Drug NameLevodopa and carbidopa (Sinemet)
DescriptionLevodopa is a metabolic precursor of dopamine. Few reports of its use in combination with carbidopa (vide infra) in NMS exist because of its dopaminergic action. Crosses the blood-brain barrier and is converted to dopamine by enzyme action, thus restoring dopamine levels in the extrapyramidal centers such as substantia nigra.
Carbidopa, a dopamine decarboxylase inhibitor, does not cross the blood-brain barrier. Diminishes the metabolism of levodopa in the GI tract and peripheral tissues, thus increasing levodopa's availability in the CNS and enhancing its effectiveness.
A variety of dosage ratios are available (ie, 1:10 carbidopa to levodopa, 1:4 carbidopa to levodopa). Also available as IR and SR dosage forms.
Adult Dose25 (carbidopa)/250 (levodopa) mg PO tid/qid
Alternatively, 500-1000 (based on levodopa component) mg/d PO divided q6-12h; increase by 100-750 mg/d q3-7d until response; not to exceed 8000 mg/d
Pediatric DoseNot established
ContraindicationsDocumented hypersensitivity; narrow-angle glaucoma; malignant melanoma; undiagnosed skin lesions
InteractionsAntacids increase bioavailability of levodopa; benzodiazepines, hydantoins, methionine, papaverine, and pyridoxine decrease levodopa effectiveness; iron salts and anticholinergics decrease GI absorption of levodopa; MAOIs may increase hypertensive reaction; may decrease metoclopramide effects; methyldopa may have additive hypotensive effects
PregnancyC - Safety for use during pregnancy has not been established.
PrecautionsCaution with severe cardiovascular or pulmonary disease, asthma, occlusive cerebrovascular disease, renal or hepatic or endocrine disease, affective disorders, major psychoses, cardiac arrhythmias, and chronic wide-angle glaucoma


FOLLOW-UP

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Deterrence/Prevention

  • Because NMS usually develops while the dose is being increased, be alert to this possibility until a steady dose is achieved.
  • Know the risk factors and be vigilant for NMS development.

Complications

  • Respiratory failure
  • Aspiration pneumonia
  • Renal failure
  • Cardiovascular collapse and arrhythmias
  • Thromboembolism and DIC

Prognosis

  • Prognosis depends on how early patient is treated and on the presence of such associated complications as respiratory or renal failure.
  • The mortality rate once reported at 20-30% is now estimated at 5-11.6%.
  • The mortality rate rises to about 50% if NMS is complicated by renal failure.

Patient Education

  • Explain and educate the patient and caretakers about possible adverse effects of medications.


MISCELLANEOUS

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Medical/Legal Pitfalls

  • Several other drugs in addition to neuroleptics can cause this potentially lethal condition.
  • Know the risk factors for NMS if a patient must be started on neuroleptics.
  • Monitor the patient on close follow-up in the outpatient department while the dose of neuroleptics is being increased.
  • Explain this serious complication of the therapy to the patient and the patient's caregiver.
  • Explore the possibility of a recent neuroleptic administration in any patient who presents with the symptom complex of hyperthermia, rigidity, and altered mentation. Necessary investigations may be performed to rule out other treatable and potentially serious conditions that could cause similar symptomatology.
  • Treatment is mainly supportive; it is directed toward controlling the rigidity and hyperthermia and toward preventing other complications (eg, respiratory failure, renal failure). Remember that development of renal failure increases the mortality rate to 50%.


REFERENCES

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  • Addonizio G, Susman VL. ECT as a treatment alternative for patients with symptoms of neuroleptic malignant syndrome. J Clin Psychiatry. Mar 1987;48(3):102-5. [Medline].
  • Bismuth C, de Rohan-Chabot P, Goulon M, Raphael JC. Dantrolene--a new therapeutic approach to the neuroleptic malignant syndrome. Acta Neurol Scand Suppl. 1984;100:193-8. [Medline].
  • Cawrse N, Wilson S, Williams M, Burge T. Neuroleptic malignant syndrome in the burns patient?. Burns. Aug 2006;32(5):647-9. [Medline].
  • Demirkiran M, Jankovic J, Dean JM. Ecstasy intoxication: an overlap between serotonin syndrome and neuroleptic malignant syndrome. Clin Neuropharmacol. Apr 1996;19(2):157-64. [Medline].
  • Ellenhorn MJ, Schonwald S, Ordog G. Ellenhorn's Medical Toxicology: Diagnosis and Treatment of Human Poisoning. 2nd ed. Baltimore, Md:. Williams & Wilkins;1997:663-664, 1187-1190.
  • Haddad LM, Shannon MW, Winchester JF. Clinical Management of Poisoning and Drug Overdose. 3rd ed. Philadelphia, Pa:. Saunders;1998:139-40, 633-34, 639-40.
  • Hammerman S, Lam C, Caroff SN. Neuroleptic malignant syndrome and aripiprazole. J Am Acad Child Adolesc Psychiatry. Jun 2006;45(6):639-41. [Medline].
  • Harsch HH. Neuroleptic malignant syndrome: physiological and laboratory findings in a series of nine cases. J Clin Psychiatry. Aug 1987;48(8):328-33. [Medline].
  • Hasan S, Buckley P. Novel antipsychotics and the neuroleptic malignant syndrome: a review and critique. Am J Psychiatry. Aug 1998;155(8):1113-6. [Medline][Full Text].
  • Khan HM, Syed NA, Sheerani M, et al. Neuroleptic malignant syndrome: need for early diagnosis and therapy. J Ayub Med Coll Abbottabad. Jan-Mar 2006;18(1):17-21. [Medline].
  • Koponen H, Repo E, Lepola U. Long-term outcome after neuroleptic malignant syndrome. Acta Psychiatr Scand. Dec 1991;84(6):550-1. [Medline].
  • Labuda A, Cullen N. Brain injury following neuroleptic malignant syndrome: Case report and review of the literature. Brain Inj. Jun 2006;20(7):775-8. [Medline].
  • Mohan KS, Gangadhar BN, Pradhan N, Channabasavanna SM. Malignant neuroleptic syndrome. J Indian Med Assoc. Dec 1985;83(12):410-3. [Medline].
  • Moore A, O''Donohoe NV, Monaghan H. Neuroleptic malignant syndrome. Arch Dis Child. Aug 1986;61(8):793-5. [Medline].
  • Naganuma H, Fujii I. Incidence and risk factors in neuroleptic malignant syndrome. Acta Psychiatr Scand. Dec 1994;90(6):424-6. [Medline].
  • Supe S, Matijevic V, Kondic L, Alvir D. Series of seizures as a sign of development of recurrent malignant neuroleptic syndrome - a case report. Psychiatr Danub. Jun 2006;18(1-2):97-101. [Medline].
  • Susman VL, Addonizio G. Recurrence of neuroleptic malignant syndrome. J Nerv Ment Dis. Apr 1988;176(4):234-41. [Medline].
  • Taketomo CK, Hodding JH, Kraus DM. Pediatric Dosage Handbook. 6th ed. Hudson, Ohio:. Lexi-Comp;1999.
  • Tanii H, Ichihashi K, Inoue K, et al. Possible neuroleptic malignant syndrome related to concomitant treatment with paroxetine and alprazolam. Prog Neuropsychopharmacol Biol Psychiatry. Aug 2006;30(6):1176-8. [Medline].
  • Turk J, Lask B. Neuroleptic malignant syndrome. Arch Dis Child. Jan 1991;66(1):91-2. [Medline].
  • van Harten PN, Kemperman CJ. Organic amnestic disorder: a long-term sequel after neuroleptic malignant syndrome. Biol Psychiatry. Feb 15 1991;29(4):407-10. [Medline].

Neuroleptic Malignant Syndrome excerpt

Article Last Updated: Aug 14, 2006