Your search keyword '"Hoyte, Christopher O."' showing total 2 results

1. Cardiac sodium channel blockade after an intentional ingestion of lacosamide, cyclobenzaprine, and levetiracetam: Case report.

Author

Chua-Tuan JL, Cao D, Iwanicki JL, and Hoyte CO

Subjects

Acetamides blood, Adolescent, Amitriptyline poisoning, Anticonvulsants blood, Drug Interactions, Drug Overdose, Electrocardiography, Female, Heart Arrest diagnosis, Heart Arrest metabolism, Heart Arrest therapy, Humans, Lacosamide, Levetiracetam, Piracetam poisoning, Risk Factors, Sodium Bicarbonate therapeutic use, Sodium Channels metabolism, Suicide, Attempted, Tachycardia, Ventricular diagnosis, Tachycardia, Ventricular metabolism, Tachycardia, Ventricular therapy, Treatment Outcome, Acetamides poisoning, Amitriptyline analogs & derivatives, Anticonvulsants poisoning, Epilepsy drug therapy, Heart Arrest chemically induced, Piracetam analogs & derivatives, Sodium Channel Blockers poisoning, Sodium Channels drug effects, Tachycardia, Ventricular chemically induced

Abstract

Context: Lacosamide treats partial seizures by enhancing slow inactivation of voltage-gated sodium channels. The described cardiac toxicity of lacosamide in the literature to date includes atrioventricular blockade (PR prolongation), atrial flutter, atrial fibrillation, sinus pauses, ventricular tachycardia and a single cardiac arrest. We report a second case of cardiac arrest following an intentional lacosamide overdose., Case Details: A 16 year-old female with a seizure disorder was found unresponsive in pulseless ventricular tachycardia after intentionally ingesting 4.5 g (76 mg/kg) lacosamide, 120 mg (2 mg/kg) cyclobenzaprine and an unknown amount of levetiracetam. Exact time of ingestion was unknown. Her initial electrocardiogram (ECG) demonstrated sinus tachycardia at 139 beats per minute, QRS duration 112 ms, and terminal R-wave in lead aVR > 3 mm. Despite treatment with 150 mEq of sodium bicarbonate, she had persistent EKG findings eight hours after presentation. Her serum lacosamide concentration nine hours after presentation was elevated at 22.8 μg/mL, while serum cyclobenzaprine concentration was 16 ng/mL (therapeutic: 10-30 ng/mL), and serum levetiracetam concentration was 22.7 μg/mL (therapeutic: 12-46 μg/mL). On hospital day three, ECG demonstrated resolution of the terminal R-wave with QRS of 78 ms. The patient recovered without physical or neurologic sequelae., Discussion: The patient's lacosamide, cyclobenzaprine and levetiracetam overdose was associated with QRS prolongation and terminal right axis deviation--suggesting sodium channel blockade as a likely etiology for her cardiac arrest. Cyclobenzaprine has potential for sodium channel blockade and ventricular dysrhythmias although cardiac toxicity due to cyclobenzaprine alone is rare. The combination of cyclobenzaprine with lacosamide may have resulted in cardiovascular collapse. In conclusion, overdose of lacosamide combined with therapeutic concentrations of sodium channel blocking xenobiotics may cause cardiac conduction delays and cardiac arrest.

Published

2015

2. 2023 American Heart Association Focused Update on the Management of Patients With Cardiac Arrest or Life-Threatening Toxicity Due to Poisoning: An Update to the American Heart Association Guidelines for Cardiopulmonary Resuscitation and Emergency Cardiovascular Care.

Author

Lavonas, Eric J., Akpunonu, Peter D., Arens, Ann M., Babu, Kavita M., Cao, Dazhe, Hoffman, Robert S., Hoyte, Christopher O., Mazer-Amirshahi, Maryann E., Stolbach, Andrew, St-Onge, Maude, Thompson, Trevonne M., Wang, George Sam, Hoover, Amber V., and Drennan, Ian R.

Subjects

*SODIUM channel blockers, *CARDIOPULMONARY resuscitation, *CARDIAC arrest, *POISONING, *CARDIAC patients

Abstract

In this focused update, the American Heart Association provides updated guidance for resuscitation of patients with cardiac arrest, respiratory arrest, and refractory shock due to poisoning. Based on structured evidence reviews, guidelines are provided for the treatment of critical poisoning from benzodiazepines, β-adrenergic receptor antagonists (also known as β-blockers), L-type calcium channel antagonists (commonly called calcium channel blockers), cocaine, cyanide, digoxin and related cardiac glycosides, local anesthetics, methemoglobinemia, opioids, organophosphates and carbamates, sodium channel antagonists (also called sodium channel blockers), and sympathomimetics. Recommendations are also provided for the use of venoarterial extracorporeal membrane oxygenation. These guidelines discuss the role of atropine, benzodiazepines, calcium, digoxin-specific immune antibody fragments, electrical pacing, flumazenil, glucagon, hemodialysis, hydroxocobalamin, hyperbaric oxygen, insulin, intravenous lipid emulsion, lidocaine, methylene blue, naloxone, pralidoxime, sodium bicarbonate, sodium nitrite, sodium thiosulfate, vasodilators, and vasopressors for the management of specific critical poisonings. [ABSTRACT FROM AUTHOR]

Published

2023