Cerebral Perfusion Pressure Directed Therapy Following Traumatic Brain Injury and Hypotension in Swine

Creator(s)

Ajai K. Malhotra, Medical College of Virginia
John B. Schweitzer, Quillen-Dishner College of Medicine
Jerry L. Fox, Quillen-Dishner College of Medicine
Timothy C. Fabian, University of Tennessee Health Science Center
Kenneth G. Proctor, University of Miami Leonard M. Miller School of Medicine

Document Type

Article

Publication Date

9-1-2003

Description

There is a paucity of studies, clinical and experimental, attesting to the benefit of cerebral perfusion pressure (CPP) directed pressor therapy following traumatic brain injury (TBI). The current study evaluates this therapy in a swine model of TBI and hypotension. Forty-five anesthetized and ventilated swine received TBI followed by a 45% blood volume bleed. After 1 h, all animals were resuscitated with 0.9% sodium chloride equal to three times the shed blood volume. The experimental group (PHE) received phenylephrine to maintain CPP > 80 mm Hg; the control group (SAL) did not. Outcomes in the first phase (n = 33) of the study were as follows: cerebro-venous oxygen saturation (S cvO2), cerebro-vascular carbon dioxide reactivity (δScvO2), and brain structural damage (β-amyloid precursor protein [βAPP] immunoreactivity). In the second phase (n = 12) of the study, extravascular blood free water (EVBFW) was measured in the brain and lung. After resuscitation, intracranial and mean arterial pressures were >15 and >80 mm Hg, respectively, in both groups. CPP declined to 64 ± 5 mm Hg in the SAL group, despite fluid supplements. CPP was maintained at >80 mm Hg with pressors in the PHE group. PHE animals maintained better ScvO2 (p < 0.05 at 180, 210, 240, 270, and 300 min post-TBI). At baseline, 5% CO2 evoked a 16 ± 4% increase in ScvO2, indicating cerebral vasodilatation and luxury perfusion. By 240 min, this response was absent in SAL animals and preserved in PHE animals (p < 0.05). Brain EVBFW was higher in SAL animals; however, lung EVBFW was higher in PHE animals. There was no difference in βAPP immunoreactivity between the SAL and PHE groups (p > 0.05). In this swine model of TBI and hypotension, CPP directed pressor therapy improved brain oxygenation and maintained cerebro-vascular CO2 reactivity. Brain edema was lower, but lung edema was greater, suggesting a higher propensity for pulmonary complications.

Citation Information

Malhotra, Ajai K.; Schweitzer, John B.; Fox, Jerry L.; Fabian, Timothy C.; and Proctor, Kenneth G.. 2003. Cerebral Perfusion Pressure Directed Therapy Following Traumatic Brain Injury and Hypotension in Swine. Journal of Neurotrauma. Vol.20(9). 827-839. https://doi.org/10.1089/089771503322385764 PMID: 14577861 ISSN: 0897-7151