Hyperbaric oxygen does not improve cerebral function when started 2 or 4 hours after cerebral arterial gas embolism in swine

Robert P Weenink; Markus W Hollmann; Xavier C E Vrijdag; Krijn P Van Lienden; Diederick W De Boo; Markus F Stevens; Thomas M Van Gulik; Robert A Van Hulst

doi:10.1097/CCM.0b013e31828a3e00

Hyperbaric oxygen does not improve cerebral function when started 2 or 4 hours after cerebral arterial gas embolism in swine

Crit Care Med. 2013 Jul;41(7):1719-27. doi: 10.1097/CCM.0b013e31828a3e00.

Authors

Robert P Weenink¹, Markus W Hollmann, Xavier C E Vrijdag, Krijn P Van Lienden, Diederick W De Boo, Markus F Stevens, Thomas M Van Gulik, Robert A Van Hulst

Affiliation

¹ Diving Medical Center, Royal Netherlands Navy, Den Helder, The Netherlands. r.p.weenink@amc.nl

PMID: 23632435
DOI: 10.1097/CCM.0b013e31828a3e00

Abstract

Objective: Hyperbaric oxygenation is the accepted treatment for cerebral arterial gas embolism. Although earlier start of hyperbaric oxygenation is associated with better outcome, it is unknown how much delay can be tolerated before start of hyperbaric oxygenation. This study investigates the effect of hyperbaric oxygenation on cerebral function in swine when initiated 2 or 4 hours after cerebral arterial gas embolism.

Design: Prospective interventional animal study.

Setting: Surgical laboratory and hyperbaric chamber.

Subjects: Twenty-two Landrace pigs.

Interventions: Under general anesthesia, probes to measure intracranial pressure, brain oxygen tension (PbtO2), and brain microdialysis, and electrodes for electroencephalography were placed. The electroencephalogram (quantified using temporal brain symmetry index) was suppressed during 1 hour by repeated injection of air boluses through a catheter placed in the right ascending pharyngeal artery. Hyperbaric oxygenation was administered using U.S. Navy Treatment Table 6 after 2- or 4-hour delay. Control animals were maintained on an inspiratory oxygen fraction of 0.4.

Measurements and main results: Intracranial pressure increased to a mean maximum of 19 mm Hg (SD, 4.5 mm Hg) due to the embolization procedure. Hyperbaric oxygenation significantly increased PbtO2 in both groups treated with hyperbaric oxygenation (mean maximum PbtO2, 390 torr; SD, 177 torr). There were no significant differences between groups with regard to temporal brain symmetry index (control vs 2-hr delay, p = 0.078; control vs 4-hr delay, p = 0.150), intracranial pressure, and microdialysis values.

Conclusions: We did not observe an effect of hyperbaric oxygenation on cerebral function after a delay of 2 or 4 hours. The injury caused in our model could be too severe for a single session of hyperbaric oxygenation to be effective. Our study should not change current hyperbaric oxygenation strategies for cerebral arterial gas embolism, but further research is necessary to elucidate our results. Whether less severe injury benefits from hyperbaric oxygenation should be investigated in models using smaller amounts of air and clinical outcome measures.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Animals
Electroencephalography
Embolism, Air / physiopathology
Embolism, Air / therapy*
Female
Hyperbaric Oxygenation / methods*
Intracranial Embolism / physiopathology
Intracranial Embolism / therapy*
Intracranial Pressure
Microdialysis
Swine
Time Factors