Abstract
Background and objectives: Loss of supraspinal cardiovascular control and secondary damage following spinal cord injury (SCI) lead to cardiovascular dysfunction, where autonomic dysreflexia (AD), triggered by stimuli below the injury, can cause uncontrolled blood pressure (BP) surges, posing severe health risks such as stroke and seizures. While anti-inflammatory neuroprotective agents have been studied for motor recovery, their impact on cardiovascular function remains under investigated. The objective was to assess the efficacy of four clinically approved neuroprotective agents in promoting cardiovascular recovery following SCI. Methods: Male Wistar rats received contusion at the third thoracic spinal segment (T3). Fluoxetine, Glyburide, Valproic acid, and Indomethacin were first administered at 1 h or 6 h post-SCI, and every 12 h for two weeks thereafter. Four weeks following SCI, hemodynamics were measured at rest and during colorectal distension. Locomotor function was assessed prior to SCI and weekly for four weeks after SCI, using the Basso-Beattie-Bresnahan (BBB) locomotor scale. Quantitative comparisons of lesion area were performed. Results: Contrary to the published literature, Indomethacin and Valproic acid resulted in high morbidity and mortality rates 60 % and 40 % respectively) within 2–3 days of administration. Fluoxetine, and Glyburide were well-tolerated. There were no differences in change in systolic BP with colorectal distension compared to control i.e., all experimental groups experienced severe episodes of AD [F(6, 67) = 0.94, p = 0.47]. There was no significant difference in BBB scores in any experimental group compared to control [F(18, 252) = 0.3, p = 0.99]. No between-group differences were observed in tissue sparing at the lesion epicentre [F(6, 422) = 6.98, p = 0.29]. Discussion: Despite promising beneficial effect reported in previous studies, none of the drugs demonstrated improvement in cardiovascular or motor function. Indomethacin and Valproic acid exhibited unexpected high mortality at doses deemed safe in the literature. This emphasizes the necessity for reproducibility studies in pre-clinical research and underscores the importance of publishing null findings to guide future investigations.
| Original language | English |
|---|---|
| Article number | 114993 |
| Journal | Experimental Neurology |
| Volume | 382 |
| DOIs | |
| State | Published - Dec 2024 |
Bibliographical note
Publisher Copyright:© 2024 The Authors
Funding
Financial support for this study was provided by the Wings for Life Spinal Cord Research Foundation Research Grant. TK is supported by a Canada Graduate Scholarship through the CIHR and a WorkSafeBC research trainee award. RS is supported by the WFLSCRF and the US Department of Defense . AK is the endowed chair in the Division of Physical Medicine and Rehabilitation within the Faculty of Medicine at the University of British Columbia and is supported through grant funding provided by WFLSCRF, International Spinal Research Trust, Praxis, US Department of Defense, RHF, Onward, SpineX, Convatec, and Coloplast. We also thank Dr. Shelly McErlane for providing expertise regarding animal welfare, and Dr. Ian Welch for the histological assessment.
| Funders | Funder number |
|---|---|
| SpineX, Convatec, and Coloplast | |
| WFLSCRF | |
| Division of Physical Medicine and Rehabilitation | |
| Wings for Life Spinal Cord Research Foundation | |
| Rose Hills Foundation | |
| Canadian Institutes of Health Research | |
| U.S. Department of Defense | |
| International Spinal Research Trust |
Keywords
- Autonomic dysreflexia
- Fluoxetine
- Glyburide
- Indomethacin
- Neuroprotection
- Spinal cord injury
- Valproic acid
ASJC Scopus subject areas
- Neurology
- Developmental Neuroscience
