4.6 Article

Retinal Ganglion Cell Damage in an Experimental Rodent Model of Blast-Mediated Traumatic Brain Injury

期刊

INVESTIGATIVE OPHTHALMOLOGY & VISUAL SCIENCE
卷 54, 期 5, 页码 3440-3450

出版社

ASSOC RESEARCH VISION OPHTHALMOLOGY INC
DOI: 10.1167/iovs.12-11522

关键词

traumatic brain injury; traumatic optic neuropathy; pattern electroretinography; blast injury

资金

  1. Department of Veterans Affairs
  2. Veterans Health Administration
  3. Office of Research and Development
  4. Rehabilitation Research and Development Center for Prevention and Treatment of Visual Loss
  5. Rehabilitation Research and Development Career Development Award
  6. RRD Merit Study Award [1I01RX000427-01]
  7. Iowa State University T32 National Institutes of Health Fellowship awards
  8. Iowa State University Biotechnology Fund

向作者/读者索取更多资源

PURPOSE. To evaluate retina and optic nerve damage following experimental blast injury. METHODS. Healthy adult mice were exposed to an overpressure blast wave using a custom-built blast chamber. The effects of blast exposure on retina and optic nerve function and structure were evaluated using the pattern electroretinogram (pERG), spectral domain optical coherence tomography (OCT), and the chromatic pupil light reflex. RESULTS. Assessment of the pupil response to light demonstrated decreased maximum pupil constriction diameter in blast-injured mice using red light or blue light stimuli 24 hours after injury compared with baseline in the eye exposed to direct blast injury. A decrease in the pupil light reflex was not observed chronically following blast exposure. We observed a biphasic pERG decrease with the acute injury recovering by 24 hours postblast and the chronic injury appearing at 4 months postblast injury. Furthermore, at 3 months following injury, a significant decrease in the retinal nerve fiber layer was observed using OCT compared with controls. Histologic analysis of the retina and optic nerve revealed punctate regions of reduced cellularity in the ganglion cell layer and damage to optic nerves. Additionally, a significant upregulation of proteins associated with oxidative stress was observed acutely following blast exposure compared with control mice. CONCLUSIONS. Our study demonstrates that decrements in retinal ganglion cell responses can be detected after blast injury using noninvasive functional and structural tests. These objective responses may serve as surrogate tests for higher CNS functions following traumatic brain injury that are difficult to quantify.

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