Pediatric Monoamine Oxidase Inhibitor Toxicity

No Results

No Results

processing….

Monoamine oxidase inhibitors (MAOIs) are a class of antidepressants that have largely fallen out of favor for the treatment of depression. However, their use is on the rise in the treatment of neurodegenerative diseases and they are still used in cases of refractory depression. ^[1]  Some antibiotics (eg, linezolid ^[2] ) are MAOIs. Although MAOI ingestion is rare, MAOI overdoses can potentially cause significant morbidity and mortality. ^[3]

Two types of monoamine oxidases are recognized: monoamine oxidase A (MAO-A) and monoamine oxidase B (MAO-B). MAO-A preferentially deaminates norepinephrine, serotonin, and dietary tyramine, whereas MAO-B mainly deaminates phenylethylamine and dopamine. MAO-B is primarily found in the basal ganglia. MAO-A is found predominantly in the liver and GI tract. MAO-A inhibitors increase the levels of norepinephrine and serotonin and are used in the treatment of clinical depression. ^{[4, 5, 6]}  MAO-B inhibitors increase the dopaminergic concentrations in the brain and have been successfully used in the treatment of Parkinson disease. ^[1]

MAOI toxicity can occur in the following three ways:

Commonly used nonselective general MAOIs include phenelzine, isocarboxazid, and tranylcypromine. MAO-A specific inhibitors include moclobemide and clorgyline. MAO-B inhibitors include pargyline and selegiline. The selegiline transdermal system has been used to decrease the risk of a dietary tyramine-induced hypertensive crisis associated with these agents.

Clinical features include hypertension, tachycardia, tremors, seizures, and hyperthermia. Because of the potential for severe toxicity and lack of effective antidotes, recognition of the disease, withdrawal of offending agents and aggressive decontamination is very important in patients with MAOI toxicity. Control of hyperthermia and fluid therapy are paramount.

Monoamine oxidase is a mitochondrial enzyme that functions to deaminate primary and secondary aromatic amines. The deamination of aromatic amines (eg, norepinephrine) leads to the compounds deactivation. MAOIs prevent the breakdown of aromatic amines in the neuronal cytosol, resulting in the storage of larger concentrations of active aromatic amines in neuronal vesicles and, therefore, an increased release of these neurotransmitters into the synaptic cleft with each action potential.

Many drugs and foods can potentiate the adrenergic and serotonergic effects of MAOIs. This characteristic is particularly important because many adverse affects involving MAOIs are due to drug-drug and drug-food interactions. ^[7]

MAOIs are rapidly absorbed and undergo first-pass metabolism in the liver. Peak plasma concentrations are achieved within 2 hours, but maximum MAO inhibition may occur 2-3 weeks later. Therefore, a washout period of at least 2 weeks when switching from MAOIs to other antidepressants (eg, tricyclic antidepressants [TCAs] and selective serotonin reuptake inhibitors [SSRIs]) is important. A lack of a washout period can trigger serotonin syndrome.

MAOIs have a narrow therapeutic window, and a dose of 2-3 mg/kg is lethal. Most cases of toxicity are related to MAO-A inhibitors.

A serious drug-related adverse effect of MAOIs is the potential to produce serotonin syndrome. Characterized by mental status changes, neuromuscular dysfunction, and autonomic instability, serotonin syndrome is thought to be secondary to excessive serotonin activity in the spinal cord and brain. Toxicity of serotonergic drugs can be caused by overdosage, interaction with other drugs, and, rarely, therapeutic doses. 

Accidental ingestion by toddlers and illicit drug use in adolescents (methylenedioxymethamphetamine [MDMA], or ecstasy) are important pediatric considerations. In adults, serotonin syndrome typically develops after the addition of a serotonergic agent to a regimen that already includes a serotonin-enhancing drug.

The mechanisms for MAOI-related toxicity can be divided into those related to MAOI overdose alone and those related to MAOI interactions with other substances.

The adverse effects related to an MAOI overdose alone can be divided into four phases, as follows:

Phase 1 is a period of latency that lasts approximately 6-12 hours; the delayed appearance of signs and symptoms is thought to be related to the gradual accumulation of norepinephrine and serotonin

Phase 2 is characterized by a catecholamine surge that causes sympathetic and CNS excitation

Phase 3 is characterized by hypotension and CNS depression 

Phase 4 involves secondary complications such as rhabdomyolysis, renal failure, pulmonary edema, myocardial infarction, and disseminated intravascular coagulopathy

Reactions caused by the interactions of MAOIs with other drugs and foods can also cause toxicity. Drug and food interactions related to MAOIs can occur at therapeutic or toxic doses. 

Foods containing tyramine can cause a hyperadrenergic state, leading to hypertension or stroke, in individuals taking MAOIs. Foods associated with MAOI interactions include the following:

​The effects of indirect-acting adrenergic drugs are markedly potentiated when combined with MAOIs; these agents include methylphenidate (Ritalin), phenylephrine, ephedrine, cocaine, and amphetamines. In contrast, direct-acting sympathomimetics such as epinephrine, norepinephrine, isoproterenol, carbidopa, and L-methyldopa directly act on the postsynaptic receptors rather than the releasing presynaptic vesicles, and they do not cause such a marked adrenergic response.

Tricyclic antidepressants (TCAs) block the inactivation of norepinephrine and serotonin ^[8] ; TCAs taken in combination with MAOIs can lead to excessive catecholamine and serotonin activity, a potentially life-threatening situation; because of the prolonged action of MAOIs, a 2-4 week washout period must be observed before treatment with TCAs is started.

Selective serotonin reuptake inhibitors (SSRIs) in conjunction with MAOIs can produce serotonin syndrome.

Similar toxicity can occur when MAOIs are combined with drugs that have serotonin reuptake inhibitory properties, such as tramadol, linezolid, meperidine, or dextromethorphan. Meperidine is known to produce significant toxicity when administered to an individual taking an MAOI. Meperidine produces a release of serotonin, which can precipitate a potentially fatal outcome.

Linezolid, an antibiotic used to treat certain drug-resistant organisms such as methicillin-resistant Staphylococcus aureus (MRSA), has been determined to be a reversible, nonselective MAOI and has been implicated in acute serotonin syndrome, usually in patients concurrently receiving SSRIs. ^[9]

Methylene blue has been reported to be associated with serotonin syndrome. It has been studied as a potent reversible MAO-A inhibitor. Analogs of methylene blue may also carry risk of serotonin syndrome. ^[10]

MAOI overdoses are rare in pediatric patients. According to the The American Association of Poison Control Centers National Poison Data System (AAPCC-NPDS), 86 single exposures to MAOIs were reported in 2017: 5 were in children under the age of 6 years; no exposures were reported in children 6 to 19 years old. ^[11]

Mortality and morbidity are dependent on the time of presentation, the occurrence of co-ingestions, and the status of the patient upon his or her arrival in the emergency department. Most patients recover without sequelae when given careful supportive care. In 2017, the AAPCC-NPDS reported 16 MAOI single exposures that resulted in moderate morbidity and 2 cases of major morbidity. There were no deaths reported. Tranylcypromine was the agent in nearly 50% of cases causing moderate to major morbidity. ^[11]

Families must be made aware of the dangers of prescription drugs, over-the-counter medications, and other potential toxins in the home. Patients who are taking MAOIs should be educated about the potential for drug and food interactions.

For excellent patient education resources, visit eMedicineHealth’s First Aid and Injuries Center and Mental Health Center. Also, see eMedicineHealth’s patient education articles Poisoning, Drug Overdose, Activated Charcoal, and Poison Proofing Your Home.

Affini A, Hagenow S, Zivkovic A, Marco-Contelles J, Stark H. Novel indanone derivatives as MAO B/H₃R dual-targeting ligands for treatment of Parkinson’s disease. Eur J Med Chem. 2018 Mar 25. 148:487-497. [Medline].

Woytowish MR, Maynor LM. Clinical relevance of linezolid-associated serotonin toxicity. Ann Pharmacother. 2013 Mar. 47(3):388-97. [Medline].

Dawson JK, Earnshaw SM, Graham CS. Dangerous monoamine oxidase inhibitor interactions are still occurring in the 1990s. J Accid Emerg Med. 1995 Mar. 12(1):49-51. [Medline].

Culpepper L. Reducing the Burden of Difficult-to-Treat Major Depressive Disorder: Revisiting Monoamine Oxidase Inhibitor Therapy. Prim Care Companion CNS Disord. 2013. 15(5):[Medline]. [Full Text].

Shulman KI, Herrmann N, Walker SE. Current place of monoamine oxidase inhibitors in the treatment of depression. CNS Drugs. 2013 Oct. 27(10):789-97. [Medline].

Fajemiroye JO, da Silva DM, de Oliveira DR, Costa EA. Treatment of anxiety and depression: medicinal plants in retrospect. Fundam Clin Pharmacol. 2016 Jun. 30 (3):198-215. [Medline]. [Full Text].

Larsen JK. MAO inhibitors: pharmacodynamic aspects and clinical implications. Acta Psychiatr Scand Suppl. 1988. 345:74-80. [Medline].

Stewart JW, Thase ME. Treating DSM-IV depression with atypical features. J Clin Psychiatry. 2007 Apr. 68(4):e10. [Medline].

Karkow DC, Kauer JF, Ernst EJ. Incidence of Serotonin Syndrome With Combined Use of Linezolid and Serotonin Reuptake Inhibitors Compared With Linezolid Monotherapy. J Clin Psychopharmacol. 2017 Oct. 37 (5):518-523. [Medline].

Delport A, Harvey BH, Petzer A, Petzer JP. The monoamine oxidase inhibition properties of selected structural analogues of methylene blue. Toxicol Appl Pharmacol. 2017 Jun 15. 325:1-8. [Medline].

Gummin DD, Mowry JB, Spyker DA, Brooks DE, Osterthaler KM, Banner W. 2017 Annual Report of the American Association of Poison Control Centers’ National Poison Data System (NPDS): 35th Annual Report. Clin Toxicol (Phila). 2018 Dec. 56 (12):1213-1415. [Medline]. [Full Text].

Bandelow B, Michaelis S, Wedekind D. Treatment of anxiety disorders. Dialogues Clin Neurosci. 2017 Jun. 19 (2):93-107. [Medline]. [Full Text].

Soumya Ganapathy, MD Department of Emergency Medicine, Beverly Hospital

Soumya Ganapathy, MD is a member of the following medical societies: American College of Emergency Physicians

Disclosure: Nothing to disclose.

Frank A Maffei, MD, FAAP Professor of Pediatrics, Geisinger Commonwealth School of Medicine; Chair of Pediatrics, Division Chief, Pediatric Critical Care, Geisinger Janet Weis Children’s Hospital

Frank A Maffei, MD, FAAP is a member of the following medical societies: American Academy of Pediatrics

Disclosure: Nothing to disclose.

Mary L Windle, PharmD Adjunct Associate Professor, University of Nebraska Medical Center College of Pharmacy; Editor-in-Chief, Medscape Drug Reference

Disclosure: Nothing to disclose.

Jeffrey R Tucker, MD Assistant Professor, Department of Pediatrics, Division of Emergency Medicine, University of Connecticut School of Medicine, Connecticut Children’s Medical Center

Disclosure: Received salary from Merck for employment.

Stephen L Thornton, MD Associate Clinical Professor, Department of Emergency Medicine (Medical Toxicology), University of Kansas Hospital; Medical Director, University of Kansas Hospital Poison Control Center; Staff Medical Toxicologist, Children’s Mercy Hospital

Stephen L Thornton, MD is a member of the following medical societies: American Academy of Clinical Toxicology, American College of Emergency Physicians, American College of Medical Toxicology

Disclosure: Nothing to disclose.

Michael E Mullins, MD Assistant Professor, Division of Emergency Medicine, Washington University in St Louis School of Medicine; Attending Physician, Emergency Department, Barnes-Jewish Hospital

Michael E Mullins, MD is a member of the following medical societies: American Academy of Clinical Toxicology, American College of Emergency Physicians

Disclosure: Received stock ownership from Johnson & Johnson for none; Received stock ownership from Savient Pharmaceuticals for none.

Timothy E Corden, MD Associate Professor of Pediatrics, Co-Director, Policy Core, Injury Research Center, Medical College of Wisconsin; Associate Director, PICU, Children’s Hospital of Wisconsin

Timothy E Corden, MD is a member of the following medical societies: American Academy of Pediatrics, Phi Beta Kappa, Society of Critical Care Medicine, Wisconsin Medical Society

Disclosure: Nothing to disclose.

Pediatric Monoamine Oxidase Inhibitor Toxicity

Research & References of Pediatric Monoamine Oxidase Inhibitor Toxicity|A&C Accounting And Tax Services
Source

Share on Facebook

Tweet

Follow us