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Is faster still better in therapeutic hypothermia?

Abstract

The rapid institution of therapeutic hypothermia after cardiac arrest has become an accepted practice. In the previous issue of Critical Care, Haugk and colleagues present a retrospective analysis of 13 years of experience with therapeutic hypothermia at their center that suggests an association between rate of cooling and less favorable neurological outcomes. The association most likely reflects easier cooling in patients more severely brain injured by their initial cardiac arrest, and should not lead clinicians to abandon or slow their efforts to achieve post-resuscitative cooling.

Conscientious clinicians will always be challenged when they try to translate the latest research into good clinical practice. It can be particularly frustrating to hear that your efforts might in fact be harmful.

In the previous issue of Critical Care, Haugk and colleagues [1] report a retrospective analysis of 13 years of therapeutic hypothermia (TH) cases, suggesting a surprising association between faster rates of cooling and less favorable neurological outcomes. Their data generate some fascinating hypotheses and opportunities for future research but clinicians would be ill-advised, based on both our understanding of pathophysiology and the growing body of published evidence, to use this study as justification to relax efforts to achieve target temperatures as quickly as possible.

Precisely how TH improves neurological outcome after cardiac arrest is not known, but the mechanism is probably multi-factorial. TH is thought to minimize the release and the effect of free radicals, excitatory neurotransmitters and protease cascades during reperfusion of ischemic brain tissue, and may decrease vasoconstriction and intravascular thrombosis leading to potential ongoing micro-ischemia [2]. TH may also amplify the release of neuroprotective proteins [3]. For any of these proposed mechanisms, initiation of TH as soon as possible following resuscitation should be preferable.

Animal models that have been used to study TH have supported early, rapid cooling [4, 5]. In fact, one of the greatest challenges of advancing animal research into the clinical realm has been the difficulty in matching the rapid induction methods achieved in the laboratory in human subjects, with the hopes of observing similar therapeutic benefits. Although no prospective, randomized clinical trials have assessed the effect of time to target temperature on neurological outcome, there are noteworthy signals from existing human trials that support a benefit to rapid cooling. Wol and colleagues [6] analyzed patients rapidly cooled using an endovascular device and showed that the time to target temperature was an independent predictor for a good outcome (odds ratio 0.69 (0.51 to 0.98)). Although underpowered, recent clinical trials of rapid cooling devices have shown trends toward survival benefit [7] and improvement in patient outcomes compared to historical controls [8].

Retrospective data reviews are fraught with potential problems, and are best used to generate hypotheses for future rigorous prospective evaluation. Despite Haugk and colleagues' efforts to control for confounders statistically, their study does not demonstrate whether it is the rate of cooling or differences in other important variables influencing neurological outcome following TH. At most, this study suggests a statistical association, but there is not sufficient biological plausibility to suggest a causal relationship. As the authors point out, their findings might well imply that greater neurological injury is predicted by more rapid achievement of cooling during TH, rather than rapid cooling itself being inherently harmful. There is a plausible argument to be made that patients with more severe anoxic injury may be easier to cool to target temperature quickly because of damage of the thermoregulatory areas of the brain. In Haugk and colleagues' population, the starting temperatures in patients with poor neurological outcomes were half a degree lower before TH was started, suggesting that these patients were already showing some degree of impaired thermoregulation.

Researchers addressing the timing of TH induction face a difficult challenge - to separate the issues of time from return-of-spontaneous-circulation to target temperature, rate of cooling, and impaired thermoregulation. This will no doubt take place in a population that will vary in time to presentation for cooling and patient factors that affect the rate of cooling. There have been tremendous advancements in the methods available to cool patients quickly; cooling rates were originally in the area of 0.32°C per hour but we can now achieve rates more than ten-times faster [8] and are in a position to question how best to cool our patients.

It is time for researchers to ask and answer these challenging questions. Until then, clinicians should continue in their efforts to cool patients post-cardiac arrest as quickly as possible.

Author's information

DH is an Associate Professor in the Department of Emergency Medicine at Queen's University and Program Director of the Critical Care training program. He is the Director of the Regional Trauma Program, Medical Director of the Kingston Resuscitation Institute at Queen's University and the Fellowship in Resuscitation medicine. DWM is an Assistant Professor in the Department of Emergency Medicine and the Critical Care Program at Queen's University, and serves on the Board of Directors for the Kingston Resuscitation Institute.

Abbreviations

TH:

therapeutic hypothermia.

References

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Correspondence to Daniel Howes.

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DH participated in a research trial funded by Life Recovery Systems. DWM declares that he has no competing interests.

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Howes, D., Messenger, D.W. Is faster still better in therapeutic hypothermia?. Crit Care 15, 162 (2011). https://doi.org/10.1186/cc10234

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