Preclinical studies suggest that argon (Ar) might diminish the neurological and myocardial damage after any hypoxic-ischemic insult. Indeed, Ar has been tested in different models of ischemic insult, at concentrations ranging from 20% up to 80%. Overall, Ar emerged as a protective agent on cells, tissues and organs, showing less cell death, reduced infarct size and faster functional recovery. More specifically, encouraging data has been reported in animal studies on cardiac arrest (CA) in which a better and faster neurological recovery was achieved when Ar was used in the post-resuscitation ventilation. More importantly, these benefits have been replicated in different studies, enrolling both small and large animals. Finally, ventilation with Ar in O2 has been demonstrated to be safe both in animals and humans. Based on this evidence, a clinical translation is advocated. Thus, the CardioPulmonary resuscitation with Argon - CPAr trial has been conceived. The trial initially started as phase I-II trial to specifically address the question about the safety of the post resuscitation Ar-treatment. The available data on the first 30 randomized patients, evaluated by the Data Safety Monitoring Board (DSMB), were considered absolutely reassuring with regard to the safety of the experimental treatment. In this perspective, the DSMB supported the continuation of the study as a phase II trial, maintaining the study protocol in all its aspects. Thus, the aim of the CPAr trial is now to evaluate efficacy in reducing post-CA neurological injury of Ar/O2 ventilation in patients resuscitated from CA.
The trial is a multicenter, randomized, controlled, single blinded, phase II and pre marketing study in patients resuscitated from Out-of-hospital cardiac arrest (OHCA). All eligible patients will be treated in full and documented compliance with the European ResuscitationCouncil (ERC)/European Society of Intensive Care Medicine (international guidelines and local post resuscitation protocols). In addition, a randomized assignment ensures a strict comparability for both the periods of data collection of safety end-points (to be assessed blindly by the events Committee): the four hours of duration of study treatment, and the longer period of possibly related clinical events during 6 months follow up.
Study Type
INTERVENTIONAL
Allocation
RANDOMIZED
Purpose
TREATMENT
Masking
SINGLE
Enrollment
120
Ventilation with Ar 70%/O2 30% in comatose patients resuscitated from OHCA with the use of an experimental mechanical ventilator.
Ospedale Policlinico San Martino di Genova
Genova, GE, Italy
RECRUITINGOspedale San Gerado
Monza, MB, Italy
RECRUITINGFondazione IRCCS Ca' Granda Ospedale Maggiore Policlinico
Milan, Milan, Italy
RECRUITINGAzienda Ospedaliero - Universitaria di Parma
Parma, Parma, Italy
NOT_YET_RECRUITINGOspedale Civile Santa Maria degli Angeli di Pordenone
Pordenone, Pordenone, Italy
RECRUITINGArcispedale Santa Maria Nuova di Reggio Emilia
Reggio Emilia, Reggio Emilia, Italy
NOT_YET_RECRUITINGFondazione Policlinico Universitario Agostino Gemelli IRCCS
Roma, RM, Italy
RECRUITINGOspedale Santa Chiara di Trento
Trento, Trento, Italy
RECRUITINGAzienda Sanitaria Universitaria Giuliano Isontina (Asugi) di Trieste
Trieste, TS, Italy
RECRUITINGNeuronal preservation
Efficacy of Argon treatment in reducing post-CA neurological injury, assessed as 48hr serum concentration of the Neuron Specific Enolase (NSE), an established biomarker of brain injury.
Time frame: 48 hours
Myocardial preservation
Ar effect on myocardial protection is assessed through measure of hs-cTnT release
Time frame: Up to 96 hours
Brain injury
Ar effect on brain injury is assessed through MRI (imaging) if patient remains comatose
Time frame: 96 hours
Survival
Effect of argon on survival after cardiac arrest (days)
Time frame: ICU discharge (assessed up to 7 days), 1-month, 6 months
Neurological recovery
Neurological functional recovery is assessed with the CPC score
Time frame: ICU discharge (assessed up to 7 days), 1-month, 6 months
Multiorgan function
Multiorgan function is assessed through the evaluation of sequential organ failure assessment score (SOFA). The score sequentially assesses the presence and severity of dysfunctions in six organ systems: respiratory, cardiovascular, coagulation, hepatic, neurological and renal scoring 0 to 4 points per each one of the following: PaO2-fiO2 ratio; Mean arterial pressure (mmHg) or vasoactive treatment; Creatinine (mg/dL) or 24-h diuresis (ml/24h); Platelet count (x103/mm3); Serum bilirubin (mg/dL); Glasgow coma scale The following markers are also assessed: transaminases (UI/L) Pancreatic amilase, lipase (UI/L)
Time frame: Up to 96 hours
Incidence of Treatment-Emergent Adverse Events
The incidence, the timing, and the duration of the need to stop Ar 70% treatment in order to maintain the SPO2\> 90%. The incidence of potentially Ar-attributable hemodynamic adverse events (i.e. arterial hypotension not responsive to fluids and/or vasoactive/inotropic drugs).
Time frame: 1 month
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