Category: Resuscitation

Modern resuscitation has many components – emphasis on pre-hospital CPR, distribution of defibrillators, cardiac catheterization … and hypothermia.  And, now we’re not so sure about that last one.

Therapeutic hypothermia is based on two randomized trials, published in 2002, enrolling a grand total of 352 patients.  Recommendations include rapid cooling after emergency stabilization to a target temperature between 32° and 34°C, and subsequent adoption of this practice spawned a cottage industry of expensive, specialized cooling devices.  But, these temperature targets were always somewhat arbitrary, and the question persisted as to whether lower temperatures in fact conferred a neurologic survival advantage.

Nope.

Enrolling nearly a thousand patients, this randomized trial of out-of-hospital cardiac arrest randomized half to 33°C and half to 36°C.  Groups were well-balanced on typically expected features favoring survival – comorbidities, bystander CPR, arrest rhythm, and follow-up treatment.  And, after cooling for 24 hours, no difference was detected in early deaths, late deaths, or in any measure of cerebral or functional performance.  One impressive feature of this trial is the standardized withdrawal of care criteria, reducing patient heterogeneity through that mechanism.

None of this says “hypothermia doesn’t work”.  But, a sense of lacking in terms of a dose-response relationship between hypothermia and neurologic survival causes some concern.  Why did we observe such profound benefit in the early trials?  Erroneous rejection of the null hypothesis due to poor statistical power, unmeasured confounders, or something more sinister?  Adding in the pre-hospital hypothermia study from JAMA, both dose-dependent and time-dependent effects are now less certain.

The utility of hypothermia following ischemic insult seems biologically plausible, but, as the editorial comments, perhaps it’s not so much hypothermia as the maintenance of normothermia.  Already part of modern post-stroke care, treating and preventing fever improves outcomes – it may simply be the observed benefits are due to intensive antipyresis, rather than hypothermia.

It seems still reasonable to use gentle cooling as a prophylaxis against hyperthermia, but more importantly, it is time, yet again, to reflect on how better evidence refines established practice.  Without continuing to recognize the limitations of our knowledge, we must caution ourselves against rushing to generalize implementation from small sample sizes (see: tPA in acute ischemic stroke).

“Targeted Temperature Management at 33°C versus 36°C after Cardiac Arrest”
http://www.nejm.org/doi/full/10.1056/NEJMoa1310519

“Temperature Management and Modern Post–Cardiac Arrest Care”
http://www.nejm.org/doi/full/10.1056/NEJMe1312700

Considering we’re still mighty skeptical regarding the ill effects of epinephrine on coronary and cerebral blood flow during resuscitation, I have to say I’m a little doubtful regarding the addition of a second vasopressor, along with steroids.

But, these authors, building on their prior work, attempt a randomized, placebo-controlled evaluation of epinephrine versus a combination of epinephrine, vasopressin, and methylprednisolone – along with a 7-day course of additional stress-dose steroids vs. placebo if post-ROSC hypotension was observed.  At hospital discharge, there were over twice as many neurologically intact survivors in the combination group as the epinephrine group – 18/130 vs. 7/138 – and thusly the authors conclude:

“Among patients with cardiac arrest requiring vasopressors, combined vasopressin-epinephrine and methylprednisolone during CPR and stress-dose hydrocortisone in postresuscitation shock, compared with epinephrine/saline placebo, resulted in improved survival to hospital discharge with favorable neurological status.”

Regrettably, with such a concisely worded conclusion, the authors devote barely two sentences to their limitations.  Indeed, for a study with so much to discuss, the authors compose a discussion section that occupies far less than even a full page.

There are a couple glaring problems with this study – not the least of which are the baseline differences between groups.  Despite randomization, the epinephrine group was saddled with quite different causes of cardiac arrest, almost certainly favoring the intervention group.  A randomization of additional patients with hypotension as their primary cause of arrest to the steroid group is almost certainly an allocation of a more favorable cohort, whereas “metabolic” causes of arrest are probably not corticosteroid deficient.  Similarly, the epinephrine group had far more asystole than the combination group – another poor prognostic feature.  Indeed, in their multivariate logistric regression (supplemental appendix), the cause of arrest and initial rhythm had statistically similar association with good outcome as intervention group membership.

The second issue is the problem of multiple interventions.  It is not clear whether the observed effect, if present, is secondary to the vasopressin-epinephrine-methylprednisolone cocktail during resuscitation or the stress-dose hydrocortisone given to nearly all survivors of the intervention group.  55% of the epinephrine group is alive 4 hours after ROSC vs. 66% of the intervention group, which, along with their physiologic data, implies the resuscitation intervention has some treatment effect.  Then, it’s unclear what favorable effect the stress-dose steroids has – particularly considering some of the epinephrine-only group then received open-label stress-dose hydrocortisone.  After resuscitation, different numbers of each group underwent PCI and similar numbers in each group received therapeutic hypothermia – but not all, leading to potential further confounding through selection bias.

Ultimately, it’s a mess – and it’s difficult to generalize these findings from a heterogenous and unbalanced cohort to routine practice.  The authors should be applauded for their ambitious goals, but a larger study, with a more effective randomization protocol, is yet needed.

“Vasopressin, Steroids, and Epinephrine and Neurologically Favorable Survival After In-Hospital Cardiac Arrest”
www.ncbi.nlm.nih.gov/pubmed/23860985‎

Lidocaine as adjunctive treatment following cardiac arrest in the context of ventricular fibrillation/ventricular tachycardia has generally fallen out of favor and been replaced with amiodarone, a result of historical data and more recent trials.  However, the quality of the evidence is generally poor, and confounders are frequent.

So, here’s some more chaotic, retrospective evidence gathered over the course of 16 years.  This is the King County registry of OHCA, of which 1,721 patients with VF/VT and ROSC were identified.  Of these, 1296 patients received prophylactic lidocaine after ROSC, in theory, to prevent re-occurrence of VF/VT.  And, in both their unadjusted, adjusted, and propensity matched cohorts, there was a reduction in recurrence of VT/VF.  However, in their propensity-matched cohort – which may or may not be a better tool for comparing two groups than their multivariate adjustment – there was no difference in admission rate or survivors to hospital discharge.

At the least, as these authors suggest, this data provides the clinical equipoise needed to justify prospective OHCA trials exempt from informed consent.

“Prophylactic lidocaine for post resuscitation care of patients with out-of-hospital ventricular fibrillation cardiac arrest”
www.ncbi.nlm.nih.gov/pubmed/23743237‎