AI Article Synopsis

  • There is currently no effective drug treatment for spinal cord injuries, prompting research into using existing medications like imatinib for acute treatment.
  • Imatinib shows promise in improving hind limb locomotion and bladder recovery even when treatment starts up to 24 hours after injury, without causing hypersensitivity in subjects.
  • The study identifies potential biomarkers—specific cytokines/chemokines—that could indicate the effectiveness of imatinib treatment in spinal cord injury, supporting the need for further clinical trials.

Article Abstract

With no currently available drug treatment for spinal cord injury, there is a need for additional therapeutic candidates. We took the approach of repositioning existing pharmacological agents to serve as acute treatments for spinal cord injury and previously found imatinib to have positive effects on locomotor and bladder function in experimental spinal cord injury when administered immediately after the injury. However, for imatinib to have translational value, it needs to have sustained beneficial effects with delayed initiation of treatment, as well. Here, we show that imatinib improves hind limb locomotion and bladder recovery when initiation of treatment was delayed until 4 h after injury and that bladder function was improved with a delay of up to 24 h. The treatment did not induce hypersensitivity. Instead, imatinib-treated animals were generally less hypersensitive to either thermal or mechanical stimuli, compared with controls. In an effort to provide potential biomarkers, we found serum levels of three cytokines/chemokines--monocyte chemoattractant protein-1, macrophage inflammatory protein (MIP)-3α, and keratinocyte chemoattractant/growth-regulated oncogene (interleukin 8)--to increase over time with imatinib treatment and to be significantly higher in injured imatinib-treated animals than in controls during the early treatment period. This correlated to macrophage activation and autofluorescence in lymphoid organs. At the site of injury in the spinal cord, macrophage activation was instead reduced by imatinib treatment. Our data strengthen the case for clinical trials of imatinib by showing that initiation of treatment can be delayed and by identifying serum cytokines that may serve as candidate markers of effective imatinib doses.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC4752188PMC
http://dx.doi.org/10.1089/neu.2014.3863DOI Listing

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