Abstract
Cannabinoid Hyperemesis Syndrome (CHS) is characterized by recurrent, paroxysmal episodes of nausea, vomiting, and abdominal discomfort in chronic cannabis users. Optimized CHS treatment data remain limited. Recent prospective evidence have demonstrated haloperidol superiority over ondansetron. Retrospective data suggest the utility of droperidol, a dopamine antagonist like haloperidol, for treating acute CHS. To prospectively assess the utility of droperidol plus diphenhydramine to mitigate common CHS symptoms. This was a multicenter, prospective interventional study in the emergency department (ED). Participants were administered a study regimen of droperidol and diphenhydramine to treat CHS after enrollment. The primary outcome measure was the change in VAS scores within the droperidol prospective cohort. Symptoms of nausea, vomiting, and abdominal pain were measured using a visual analogue scale (VAS) up to 120minutes. Secondary measures assessed include repeat visits to the ED within seven days. Amongst 47 droperidol participants, VAS for nausea and vomiting declined from baseline 8.3±2.0 to 3.1±3.3 at 30minutes post treatment (p < 0.05), and 1.4±2.4 at 120minutes (p < 0.05). For abdominal pain, VAS mean was 7.8±2.4 at baseline declining to 3.6±2.9 at 30minutes (p < 0.05) and 1.7±2.9 at 120minutes (p < 0.05). Return to the ED within 7 days following droperidol was 12.9% (n=47). This trial shows significant improvement in symptoms from baseline, 30 and 120minutes post-treatment and return to the ED within a week post treatment with the study regimen.
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