Pharmacological postconditioning with sevoflurane after cardiopulmonary resuscitation reduces myocardial dysfunction

Meybohm, Patrick; Gruenewald, Matthias; Albrecht, Martín; Müller, Christina; Zitta, Karina; Foesel, Nikola; Maracke, Moritz; Tacke, Sabine; Schrezenmeir, Jürgen; Scholz, Jens; Bein, Berthold

doi:10.1186/cc10496

Cited by 29 publications

(18 citation statements)

References 46 publications

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“…45 This may also be the reason why some previously conducted studies were unable to find an improvement in neurological deficit score or cerebral cellular and molecular pathways when the anaesthetic was given after achievement of ROSC in a pig model of cardiac arrest for only 8 min. 37,46 Whether noble gases differ in this context and provide neurologic and myocardial protection when given later is the subject of ongoing research. 37,39 Certainly, due to their anaesthetic effects volatile anaesthetics require a tight seal and greater caution and need to be scavenged to avoid environmental contamination and potential danger to the emergency personnel when compared to noble gases.…”

Section: Discusssionmentioning

confidence: 99%

Anaesthetic Postconditioning at the Initiation of CPR Improves Myocardial and Mitochondrial Function in a Pig Model of Prolonged Untreated Ventricular Fibrillation

et al. 2014

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Background Anaesthetic postconditioning (APoC) attenuates myocardial injury following coronary ischaemia/reperfusion. We hypothesised that APoC at the initiation of cardiopulmonary resuscitation (CPR) will improve post resuscitation myocardial function along with improved mitochondrial function in a pig model of prolonged untreated ventricular fibrillation. Methods In 32 pigs isoflurane anaesthesia was discontinued prior to induction of ventricular fibrillation that was left untreated for 15 min. At the initiation of CPR, 15 animals were randomised to controls (CON), and 17 to APoC with 2 Vol% sevoflurane during the first 3 min CPR. Pigs were defibrillated after 4 min of CPR. After return of spontaneous circulation (ROSC), isoflurane was restarted at 0.8-1.5 Vol% in both groups. Systolic and diastolic blood pressures were measured continuously. Of the animals that achieved ROSC, 8 CON and 8 APoC animals were randomised to have their left ventricular ejection fraction (LVEF%) assessed by echocardiography at 4 hrs. Seven CON and 9 APoC were randomised to euthanasia 15 min after ROSC to isolate mitochondria from the left ventricle for bioenergetic studies. Results ROSC was achieved in 10/15 CON and 15/17 APoC animals. APoC improved haemodynamics during CPR and post-CPR LVEF%. Mitochondrial ATP synthesis, coupling of oxidative phosphorylation and calcium retention capacity were improved in cardiac mitochondria isolated after APoC. Conclusions In a porcine model of prolonged untreated cardiac arrest, APoC with inhaled sevoflurane at the initiation of CPR, is associated with preserved mitochondrial function and improved post resuscitation myocardial dysfunction.

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Section: Discusssionmentioning

confidence: 99%

Anaesthetic Postconditioning at the Initiation of CPR Improves Myocardial and Mitochondrial Function in a Pig Model of Prolonged Untreated Ventricular Fibrillation

et al. 2014

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“…Though the specific mechanisms remain unclear, sevoflurane has previously been shown to improve myocardial function, prevent apoptosis, and reduce cytokine production post-cardiac arrest [14]. …”

Section: Discussionmentioning

confidence: 99%

“…Ischemic postconditioning, which utilizes structured pauses in CPR, was shown to improve left ventricular ejection fraction (LVEF) and neurologically intact survival in a porcine model of cardiac arrest including 15 minutes of untreated VF [12]. Sevoflurane has been shown to reduce release of cardiac biomarkers, reduce apoptosis, and improve LVEF; however, no difference in neurologic function was reported [13, 14]. Poloxamer 188 (P188) is a nonionic copolymer thought to adhere to gaps in the cell membrane, thereby blocking pores caused by severe cellular stress [15].…”

Section: Introductionmentioning

confidence: 99%

Bundled postconditioning therapies improve hemodynamics and neurologic recovery after 17min of untreated cardiac arrest

Bartos¹,

Matsuura²,

Sarraf³

et al. 2015

Resuscitation

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Objective Ischemic postconditioning (stutter CPR) and sevoflurane have been shown to mitigate the effects of reperfusion injury in cardiac tissue after 15 minutes of ventricular fibrillation (VF) cardiac arrest. Poloxamer 188 (P188) has also proven beneficial to neuronal and cardiac tissue during reperfusion injury in human and animal models. We hypothesized that the use of stutter CPR, sevoflurane, and P188 combined with standard advanced life support would improve post-resuscitation cardiac and neurologic function after prolonged VF arrest. Methods Following 17 minutes of untreated VF, 20 pigs were randomized to Control treatment with active compression/decompression (ACD) CPR and impedance threshold device (ITD) (n=8) or Bundle therapy with stutter ACD CPR + ITD + sevoflurane + P188 (n=12). Epinephrine and post-resuscitation hypothermia were given in both groups per standard protocol. Animals that achieved return of spontaneous circulation (ROSC) were evaluated with echocardiography, biomarkers, and a blinded neurologic assessment with a cerebral performance category score. Results Bundle therapy improved hemodynamics during resuscitation, reduced need for epinephrine and repeated defibrillation, reduced biomarkers of cardiac injury and end-organ dysfunction, and increased left ventricular ejection fraction compared to Controls. Bundle therapy also improved rates of ROSC (100% vs. 50%), freedom from major adverse events (50% vs. 0% at 48 hours), and neurologic function (42% with mild or no neurologic deficit and 17% achieving normal function at 48 hours). Conclusions Bundle therapy with a combination of stutter ACD CPR, ITD, sevoflurane, and P188 improved cardiac and neurologic function after 17 minutes of untreated cardiac arrest in pigs.

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“…Although its exact signaling mechanisms are still unclear, postconditioning likely includes activation of the reperfusion injury salvage kinase and survival activating factor enhancement pathways, and result in reduced apoptosis and improved cardiac and neurologic function and eventually increased survival in different animal models of cardiac arrest [67]. For example, the introduction of several short well-defined pauses limited to only the very beginning of CPR [68], or the very early administration of pharmacologic agents [69–71] to trigger postconditioning pathways show highly promising results in the experimental setting. Before their translation into clinical practice, however, conclusive clinical trials are needed to understand and validate their benefit in humans.…”

Section: Experimental Postconditioning To Ameliorate Global Ischemia-mentioning

confidence: 99%

New Developments in Cardiac Arrest Management

Riess

2016

Advances in Anesthesia

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Pharmacological postconditioning with sevoflurane after cardiopulmonary resuscitation reduces myocardial dysfunction

Cited by 29 publications

References 46 publications

Anaesthetic Postconditioning at the Initiation of CPR Improves Myocardial and Mitochondrial Function in a Pig Model of Prolonged Untreated Ventricular Fibrillation

Anaesthetic Postconditioning at the Initiation of CPR Improves Myocardial and Mitochondrial Function in a Pig Model of Prolonged Untreated Ventricular Fibrillation

Bundled postconditioning therapies improve hemodynamics and neurologic recovery after 17min of untreated cardiac arrest

New Developments in Cardiac Arrest Management

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