Episode 1 - Toxicology

In this exciting episode, we will be discussing the role of DigiFab in chronic digoxin toxicity before diving into an interesting case of organophosphate poisoning and, to finish, we will explore whether there is a link between antipsychotic use and increased risk of MI.
Theme
Toxicology.
 
Participants
Dr Satish Mitter, Pramod Chandru, Samoda Wilegoda Mudalige, Kit Rowe, Rachel Ng, Shreyas Iyer, and Caroline Tyers.


Discussion 1:
“Clinical outcomes from early use of digoxin specific antibodies versus observation in chronic digoxin poisoning (ATOM-4)”
Betty S. Chan, Geoffrey K. Isbister, Colin B. Page, Katherine Z. Isoardi, Angela L. Chiew, Katharine A. Kirby & Nicholas A. Buckley
  • The results from this study suggest no benefit from routine use of DigiFab for chronic digoxin toxicity. 
  • Clinical indications for DigiFab use include - cardiac arrest, ventricular arrhythmias or runs of ventricular ectopic complexes and bradyarrhythmias associated with hypotension. 
  • Digoxin levels should only be performed under specific circumstances (not routinely for all patients on digoxin but rather in the context of an AKI or when there is a clinical suspicion of potential toxicity). 
  • When managing chronic digoxin toxicity, correcting any precipitating factors such as volume depletion and electrolyte abnormalities is critically important.
  • Identifying patients at risk of digoxin toxicity (the typical patient is the elderly patient with multiple comorbidities) and drugs that impair digoxin toxicity (NSAIDs and diuretics) is also vital to your overall assessment. 

Discussion 2:
Case of malathion (organophosphate) poisoning. 
  • 55-year-old male found unconscious surrounded by chemicals at home. 
  • Developed clear cholinergic toxidrome, tachycardia, and hypotension in ICU.
  • Received atropine on a doubling regimen every 5 minutes: reaching 16mg (and then a continuous infusion) with improvement in his symptoms (including this tachycardia).
  • Infusion weaned after 24 hours with recurrence of hemodynamic instability requiring inotropic support and recommencement of atropine on day 3.
  • Required atropine for 31 days in total. 
 Take-Home Points:
  • The standard, routinely taught presentations for cases do not always apply: this patient was tachycardic rather than bradycardic with his organophosphate toxicity (and this tachycardia responded to atropine). 
  • Atropine for organophosphate toxicity is vital. 
  • Oximes (such as pralidoxime) are occasionally used in the treatment of organophosphate toxicity but should be discussed with toxicology specialists prior to use. 

Discussion 3:
“Use of antipsychotics and risk of myocardial infarction: a systematic review and meta‐analysis”
Zheng-he Yu, Hai-yin Jiang, Li Shao, Yuan-yue Zhou, Hai-yan Shi and Bing Ruan                            

Take-Home Points:
  • This study suggests an association between antipsychotic use and an increased risk of MI (OR 1.88). 
  • This risk appeared to be greater within the first 30 days of use (when taking daily doses); with the risk decreasing over time. 
  • There was however significant heterogeneity in the data studied. 
  • The recent commencement of an antipsychotic may be worth considering as an added risk factor for ischaemic heart disease in a patient presenting with chest pain.

Credits:
The discussions were mediated by ED consultant and toxicologist Dr Satish Mitter and ED consultant Dr Pramod Chandru.


This episode was produced by the ­­­­Emergency Medicine Training Network 5 with the assistance of Dr Kavita Varshney, Deepa Dasgupta, Cynthia De Macedo Franco, and Paul Scott.

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Thank you for listening to our first podcast episode!
Please send us an email to let us know what you thought.
You can contact us at westmeadedjournalclub@gmail.com

See you next time,
Caroline, Kit, Pramod, Samoda and Shreyas.















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