Journal
BRAIN RESEARCH
Volume 1561, Issue -, Pages 11-22Publisher
ELSEVIER SCIENCE BV
DOI: 10.1016/j.brainres.2014.03.002
Keywords
Trauma; Neuroprotection; Selective estrogen receptor modulators; 17 beta-estradiol; Locomotor recovery; Estrogen receptor expression
Categories
Funding
- COBRE [P20-GM103642]
- MBRS-RISE Program [R25-GM061838]
- MBRS-SCORE [S06-GM008224]
- RCMI Program [G12RR03051]
- Division of Biomedical Sciences of the UPR School of Medicine
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17 beta-Estradiol is a multi-active steroid that imparts neuroprotection via diverse mechanisms of action. However, its role as a neuroprotective agent after spinal cord injury (SCI), or the involvement of the estrogen receptor-alpha (ER-a) in locomotor recovery, is still a subject of much debate. In this study, we evaluated the effects of estradiol and of Tamoxifen (an estrogen receptor mixed agonist/antagonist) on locomotor recovery following SCI. To control estradiol cyclical variability, ovariectomized female rats received empty or estradiol filled implants, prior to a moderate contusion to the spinal cord. Estradiol improved locomotor function at 7, 14, 21, and 28 days post injury (DPI), when compared to control groups (measured with the BBB open field test). This effect was ER-a mediated, because functional recovery was blocked with an ER-a antagonist. We also observed that ER-a was up-regulated after SCI. Long-term treatment (28 DPI) with estradiol and Tamoxifen reduced the extent of the lesion cavity, an effect also mediated by ER-a. The antioxidant effects of estradiol were seen acutely at 2 DPI but not at 28 DPI, and this acute effect was not receptor mediated. Rats treated with Tamoxifen recovered some locomotor activity at 21 and 28 DPI, which could be related to the antioxidant protection seen at these time points. These results show that estradiol improves functional outcome, and these protective effects are mediated by the ER-a dependent and independent-mechanisms. Tamoxifen's effects during late stages of SCI support the use of this drug as a long-term alternative treatment for this condition. (C) 2014 Elsevier B.V. All rights reserved.
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