The in vivo effect of propranolol on cerebral perfusion and hypoxia after traumatic brain injury

Eric J Ley; Jeff Scehnet; Ryan Park; Stu Schroff; Grant Dagliyan; Peter S Conti; Daniel R Margulies; Ali Salim

doi:10.1097/TA.0b013e31819388be

The in vivo effect of propranolol on cerebral perfusion and hypoxia after traumatic brain injury

J Trauma. 2009 Jan;66(1):154-9; discussion 159-61. doi: 10.1097/TA.0b013e31819388be.

Authors

Eric J Ley¹, Jeff Scehnet, Ryan Park, Stu Schroff, Grant Dagliyan, Peter S Conti, Daniel R Margulies, Ali Salim

Affiliation

¹ Department of Surgery, Division of Trauma and Critical Care, Cedars-Sinai Medical Center, Los Angeles, CA 90048, USA.

PMID: 19131818
DOI: 10.1097/TA.0b013e31819388be

Abstract

Background: Recent epidemiologic evidence has identified beta-blockade as independently associated with improved survival in patients with isolated traumatic brain injury (TBI). Reduced sympathetic discharge and catecholamine release may improve circulation in the injured areas and influence delayed demise. The purpose of this study was to investigate the cerebral effect of beta-blockade in a murine TBI model using immunohistochemical and microPET analysis.

Methods: Balb/c mice underwent TBI as in a previously described model and were randomized to receive treatment with propranolol or placebo in a blinded fashion. Immunofluorescent images were obtained for vessel density (CD31), vessel perfusion (Ricinus communis agglutinin [RCA]-lectin), and cerebral hypoxia (hypoxyprobe-1) and compared by digital quantification. Perfusion measurements were acquired using positron emission tomography microPET scans with [64Cu]-pyruvaldehyde bis(N4-methylthiosemicarbazone) ([64Cu]-PTSM) and converted into standardized uptake values (SUV) for analysis.

Results: On immunohistochemical analysis, the normal mouse cerebral perfusion was a quantitated mean of 325 +/- 20, the cerebral perfusion after TBI and treatment with placebo was 113 +/- 25, and the cerebral perfusion after TBI treated with propranolol was 172 +/- 23. Immunohistochemical analysis demonstrated treatment with propranolol improved cerebral perfusion by 152% (p value <0.01) and reduced cerebral hypoxia by 24.2% (p value <0.01) compared with treatment with placebo. MicroPET imaging of the normal mouse brain after injection with placebo measured a SUV of 0.7075 +/- 0.02; the normal mouse brain after treatment with propranolol measured a SUV of 0.400 +/- 0.02. After TBI and treatment with placebo, the SUV reduced to 0.395 +/- 0.01; after treatment with propranolol the SUV measured 0.515 +/- 0.04. MicroPET imaging demonstrated propranolol improved cerebral perfusion after TBI to 130% of placebo (p value <0.01).

Conclusion: Propranolol in vivo increased cerebral perfusion and decreased cerebral hypoxia. This research demonstrates beta-blockade may prevent additional brain damage after traumatic insult and should be the focus of future clinical trials.

MeSH terms

Analysis of Variance
Animals
Brain Injuries / diagnostic imaging
Brain Injuries / drug therapy*
Cerebrovascular Circulation / drug effects*
Hypoxia / diagnostic imaging
Hypoxia / drug therapy*
Immunohistochemistry
Linear Models
Mice
Mice, Inbred BALB C
Organometallic Compounds
Propranolol / pharmacology*
Radiopharmaceuticals
Random Allocation
Statistics, Nonparametric
Thiosemicarbazones
Tomography, Emission-Computed

Substances

Organometallic Compounds
Radiopharmaceuticals
Thiosemicarbazones
copper pyruvaldehyde bis(N(4)-methylthiosemicarbazone) complex
Propranolol