4.6 Article

Extended (10-Day) Real-Time Monitoring by Dexamethasone-Enhanced Microdialysis in the Injured Rat Cortex

Journal

ACS CHEMICAL NEUROSCIENCE
Volume 10, Issue 8, Pages 3521-3531

Publisher

AMER CHEMICAL SOC
DOI: 10.1021/acschemneuro.9b00145

Keywords

Microdialysis; dexamethasone; biosensor; microfluidic; spreading depolarization; controlled cortical impact

Funding

  1. National Institutes of Health [R01NS102725, R21NS109875]
  2. University of Pittsburgh Center for Biological Imaging [1S10RR028478-01]

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Intracerebral microdialysis has proven useful for chemical monitoring in patients following traumatic brain injury. Recent studies in animals, however, have documented that insertion of microdialysis probes into brain tissues initiates a foreign-body response. Within a few days after probe insertion, the foreign body response impedes the use of microdialysis to monitor the K+ and glucose transients associated with spreading depolarization, a potential mechanism for secondary brain injury. Herein, we show that perfusing microdialysis probes with dexamethasone, a potent anti-inflammatory glucocorticoid, suppresses the foreign body response and facilitates the monitoring of spontaneous spreading depolarizations for at least 10 days following controlled cortical injury in the rat. In addition to spreading depolarizations, results of this study suggest that a progressive, apparently permanent, decline in pericontusional interstitial glucose may be an additional sequela of brain injury. This study establishes extended dexamethasone-enhanced microdialysis in the injured rodent cortex as a new paradigm for investigating trauma-induced metabolic crisis.

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