Posttraumatic midazolam administration does not influence brain damage after experimental traumatic brain injury

Anne Sebastiani; Simone Bender; Michael K E Schäfer; Serge C Thal

doi:10.1186/s12871-022-01592-x

Posttraumatic midazolam administration does not influence brain damage after experimental traumatic brain injury

BMC Anesthesiol. 2022 Mar 4;22(1):60. doi: 10.1186/s12871-022-01592-x.

Authors

Anne Sebastiani^{1

2}, Simone Bender², Michael K E Schäfer², Serge C Thal^{3

4}

Affiliations

¹ Department of Anesthesiology, HELIOS University Hospital Wuppertal, University of Witten/Herdecke, Heusnerstrasse 40, 42283, Wuppertal, Germany.
² Department of Anesthesiology, University Medical Center of the Johannes Gutenberg University, Mainz, Germany.
³ Department of Anesthesiology, HELIOS University Hospital Wuppertal, University of Witten/Herdecke, Heusnerstrasse 40, 42283, Wuppertal, Germany. serge@thal.de.
⁴ Department of Anesthesiology, University Medical Center of the Johannes Gutenberg University, Mainz, Germany. serge@thal.de.

Abstract

Background: The benzodiazepine midazolam is a γ-aminobutyric acid (GABA)-A receptor agonist frequently used for sedation or stress control in patients suffering from traumatic brain injury (TBI). However, experimental studies on benzodiazepines have reported divergent results, raising concerns about its widespread use in patients. Some studies indicate that benzodiazepine-mediated potentiation of GABAergic neurotransmission is detrimental in brain-injured animals. However, other experimental investigations demonstrate neuroprotective effects, especially in pretreatment paradigms. This study investigated whether single-bolus midazolam administration influences secondary brain damage post-TBI.

Methods: Two different midazolam dosages (0.5 and 5 mg/kg BW), a combination of midazolam and its competitive antagonist flumazenil, or vehicle solution (NaCl 0.9%) was injected intravenously to mice 24 h after experimental TBI induced by controlled cortical impact. Mice were evaluated for neurological and motor deficits using a 15-point neuroscore and the rotarod test. Histopathological brain damage and mRNA expression of inflammatory marker genes were analyzed using quantitative polymerase chain reaction three days after insult.

Results: Histological brain damage was not affected by posttraumatic midazolam administration. Midazolam impaired functional recovery, and this effect could not be counteracted by administering the midazolam antagonist flumazenil. An increase in IL-1β mRNA levels due to postinjury application of midazolam was reversible by flumazenil administration. However, other inflammatory parameters were not affected.

Conclusions: This study merely reports minor effects of a postinjury midazolam application. Further studies focusing on a time-dependent analysis of posttraumatic benzodiazepine administration are required.

Keywords: Anesthesia; Benzodiazepines; Controlled cortical impact; Flumazenil; Midazolam; Neurological function; Neurotoxicity; Sedation; Traumatic brain injury; γ-aminobutyric acid-A receptor.

MeSH terms

Animals
Benzodiazepines
Brain
Brain Injuries* / drug therapy
Brain Injuries, Traumatic* / complications
Brain Injuries, Traumatic* / drug therapy
Flumazenil / adverse effects
Humans
Mice
Midazolam
RNA, Messenger

Substances

RNA, Messenger
Benzodiazepines
Flumazenil
Midazolam