Pulseless electrical activity risk factors

Resident Survival Guide

Editor-In-Chief: C. Michael Gibson, M.S., M.D. [1]

Overview

The administration of beta blockers and calcium channel blockers is associated with an increased risk of PEA. This may be due to their effect on Ca / troponin interactions, and their inhibition of myocardial contractility. History of syncope and pulmonary disease is also associated with a higher risk of presenting PEA ^[1], as well as history of syncope.

Risk Factors

Beta Blockers and Calcium Channel Blockers

The main interrogant rewarding whether or not Beta blockers and ACE inhibitors are risk factors for presenting PEA is to determine that they are not aiding into the conversion of VF to PEA. There has been extense literature proving a decrease in the incidence of VF. However, there is a need to determine whether the relative numbers of the increase of PEA as the presenting rhythm in sudden cardiac arrest are not in fact increasing because of the decrease of VF due to pharmacological treatment with beta blockers and ACE inhibitors. Or, that the use of beta blockers and ACE inhibitors is diminishing the prevalence of VF, on the behalf of converting VF to PEA or asystole.

Syncope and PEA

There is a strong correlation between patients that had a syncope episode to present future PEA, than those who didn’t. Prevalence is also higher in patients that presented PEA, than those who presented VF/VT or asystolia. Findings were consistent with an odds ratio of 2.64 (Confidence interval 1.31 to 5.32) versus VF/VT and OR of 2.27 (Confidence interval of 1.08 to 4.78) versus asystolia ^[1].

Pulmonary Disease and PEA

Teodorescu et al suggest, a strong relation between pulmonary disease and increased frequency of PEA. There are other publications supporting this association ^{[2] [3]}.

References

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