Article
Journal of Cerebral Blood Flow & Metabolism (1997) 17, 1210–1220; doi:10.1097/00004647-199711000-00010
Early White Blood Cell Dynamics After Traumatic Brain Injury: Effects on the Cerebral Microcirculation
This study was supported by the Annie Laurie Aitken Charitable Trust Fund as part of their commitment to the advancement of brain injury research. It has been presented in part at the 68th Annual Meeting of the American Association of Neurological Surgeons, Minneapolis, Minnesota, 1996.
Roger Härtl, Max B Medary, Maximilian Ruge, Karl E Arfors and Jam Ghajar
The Aitken Neuroscience Center and Cornell University Medical College, New York, New York, U.S.A.
Correspondence: Roger Härtl, Aitken Neuroscience Center, 523 E. 72nd Street, 8th Floor, New York, NY, U.S.A.
Received 21 January 1997; Revised 23 June 1997; Accepted 14 July 1997.
Abstract
Increasing clinical and experimental evidence suggests that traumatic brain injury (TBI) elicits an acute inflammatory response. In the present study we investigated whether white blood cells (WBC) are activated in the cerebral micro-circulation early after TBI and whether WBC accumulation affects the posttraumatic cerebrovascular response. Twenty-four anesthetized rabbits had chronic cranial windows implanted 3 weeks before experimentation. Animals were divided into four experimental groups and were studied for 7 hours (groups I, IIa, and III) or 2 hours (group IIb). Intravital fluorescence videomicroscopy was used to visualize WBC (rhodamine 6G, intravenously), pial vessel diameters, and blood-brain barrier (BBB) integrity (Na+-fluorescein) at 6 hours (groups I, IIa, and III) or 1 hour (group IIb) after TBI. Group I (n = 5) consisted of sham-operated animals. Groups IIa (n = 7) and IIb (n = 5) received fluid-percussion injury at 1 hour. Group III (n = 7) received fluid-percussion injury and 1 mg/kg anti-adhesion monoclonal antibody (MoAb) 5 minutes before injury. Venular WBC sticking, intracranial pressure (ICP), and arterial vessel diameters increased significantly for 6 hours after trauma. IB4 reduced WBC margination and prevented vasodilation. Intracranial pressure was not reduced by treatment with IB4. Blood-brain barrier damage occurred at 1 hour but not at 6 hours after TBI and was independent of WBC activation. This first report using intravital videomicroscopy to study the inflammatory response after TBI reveals upregulated interaction between WBC and cerebral endothelium that can be manipulated pharmacologically. White blood cell activation is associated with pial arteriolar vasodilation. White blood cells do not induce BBB breakdown less than 6 hours after TBI and do not contribute to posttraumatic ICP elevation. The role of WBC more than 6 hours after TBI should be investigated further.
Keywords:
Blood-brain barrier, Cranial window, Inflammation, Leukocytes, Microcirculation, Traumatic brain injury, Videomicroscopy
Abbreviations:
AD, arteriolar diameters; BBB, blood-brain barrier; ETCO2, end-tidal PCO2; ICP, intracranial pressure; MAP, mean arterial blood pressure; MoAb, monoclonal antibody; TBI, traumatic brain injury; WBC, white blood cell
