Efficacy of Early Intravenous High-dose Vitamin C in Post-cardiac Arrest Shock.
- Conditions
- Cardiac Arrest
- Interventions
- Drug: standard treatmentDrug: Vitamin C (Laroscorbine) + Vitamin B1 (Bevitine)
- Registration Number
- NCT05817851
- Lead Sponsor
- Centre Hospitalier de Bethune
- Brief Summary
Among patients admitted after an out-of-hospital cardiac arrest (OHCA) in intensive care unit (ICU), almost two thirds of patients will develop in the first hours a post-cardiac arrest (CA) shock. This post-CA shock, combines cardiac and hemodynamic failure, generally resulting in multi-organ failure and early death in up to 35% of patients. Experimental data suggest that intravenous ascorbic acid (vitamin C) may attenuate inflammation and vascular injury related to sepsis or surgery. Preclinical and clinical studies also provide safety data of high dose intravenous vitamin C (\> 200mg/kg/day) with no significant adverse event reported and favorable impact on outcome. Experimental data also suggest beneficial effect of vitamin C in post-CA management with improvement of shock and multi-organ failure with potential benefit on neuroprotection and outcome.
The study is a phase II multicenter prospective controlled open-label trial randomized in two parallel groups :
* Expérimental group: Standard of care care for post-CA shock + Vitamin C (Vit-C) 200mg/kg/d IV (started as early as possible, no later than 1 h after randomization + thiamin (Vit B1) 200mg every 12 h during 3 days.
* Control group: Standard of care care for post CA shock according international guidelines.
Patient number to be enrolled : 234, Study duration :24 months and 28 days, Inclusion duration : 24 months, Patient participation : duration : 28 days
- Detailed Description
Not available
Recruitment & Eligibility
- Status
- RECRUITING
- Sex
- All
- Target Recruitment
- 234
- patients still comatose (Glasgow coma scale < 8) after an OHCA of presumed cardiac origin with ROSC < 60 min;
- and treated with a norepinephrin or an epinephrin continuous infusion during at least 30 min before randomization to maintain mean arterial pressure (MAP) ≥ 65 mmHg.
- patients still comatose (Glasgow coma scale < 8) after an OHCA of presumed cardiac origin with ROSC < 60 min;
- and treated with a norepinephrin or an epinephrin continuous infusion ≥ 0.2µg/kg/h, within 4 hours after OHCA, during at least 30 min/h to maintain mean arterial pressure (MAP) ≥ 65 mmHg.
Exclusion criteria:
- minor or pregnant women;
- OHCA from evident extracardiac cause (trauma, bleeding, poisoning, etc.);
- interval between RACS and randomization > 6 hours;
- extracorporeal circulatory assistance requirement in the first 4 hours after OHCA;
- history of urolithiasis, oxalate nephropathy or hemochromatosis;
- glucose-6-phosphate deshydrogenase deficiency; nephrolithiasis, hyperoxalyurie
- patients already treated with vit-C; known vit-C deficit;
- inclusion in another study;
- pre-existent severe chronic kidney disease (glomerular filtration rate < 30ml/min);
- treatment limitationsor moribound
- Patient with derpived freedom or with legal protective measures.
- Patient not covered by French national health insurance
Study & Design
- Study Type
- INTERVENTIONAL
- Study Design
- PARALLEL
- Arm && Interventions
Group Intervention Description Control group standard treatment - Control group (standard treatment): post-cardiac arrest care will be provided, including temperature control, according to current international guidelines and local procedures. Standard IV vit-C supplementation will be allowed for dosages up to 1000 mg a day from day 4 after randomization, as well as thiamin supplementation. Experimental group Vitamin C (Laroscorbine) + Vitamin B1 (Bevitine) - Experimental group (IV high-dose vit-C): in addition of standard post-CA as the control group, patients will receive an IV high-dose vit-C 50mg/kg infusion every 6 hours, started within the hour after randomization, for 3 days. In addition, all patients will receive intravenous thiamine 200 mg twice a day for 3 days to limit the oxalate production.
- Primary Outcome Measures
Name Time Method Cumulative incidence of weaning from vasopressors at day 3 after OHCA. day 3 Cumulative incidence of weaning from vasopressors at day 3 after OHCA.
- Secondary Outcome Measures
Name Time Method Cumulative incidence of death by refractory shock within 7 days after OHCA. day 7 after OHCA Cumulative incidence of death by refractory shock within 7 days after OHCA.
the neurological outcome at day 28 after OHCA, with mRS range from 0 to 3. day 28 after OHCA Assessed using the mRS (favorable neurological outcome will be considered if mRS range from 0 to 3; Unfavorable neurological outcome will be considered if mRS range from 4 to 6).
The maximal vasopressors infusion dose within 3 days after OHCA. 72 hours after OHCA The maximal vasopressors infusion dose within 3 days after OHCA.
The delta SOFA (sepsis-related organ failure assessment score) is defined as the difference between SOFA admission and SOFA at 72 hours after OHCA. 72 hours after OHCA Death within 72 hours will be counted as the maximum SOFA score (i.e. 24 points).
The lower arterial lactate level at day 3 after OHCA. 72 hours after OHCA The lower arterial lactate level at day 3 after OHCA.
Trial Locations
- Locations (10)
Centre Hospitalier de Rouen
🇫🇷Rouen, France
Centre Hospitalier Universitaire d'Amiens
🇫🇷Amiens, France
Centre Hospitalier Béthune
🇫🇷Béthune, France
Centre Hospitalier de Dieppe
🇫🇷Dieppe, France
GHEF Site Marne La Vallée
🇫🇷Jossigny, France
Centre Hospitalier de LENS
🇫🇷Lens, France
Centre Hospitalier Universitaire de LILLE
🇫🇷Lille, France
Hôpital Lariboisière
🇫🇷Paris, France
Centre Hospitalier Toulon La Seyne sur Mer
🇫🇷Toulon, France
Centre Hospitalier de Valenciennes
🇫🇷Valenciennes, France