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Attenuation of Corpus Callosum Axon Myelination and Remyelination in the Absence of Circulating Sex Hormones

Authors :
Daniel K. Crawford
Gemmy Hannsun
Spencer M. Moore
Seema K. Tiwari-Woodruff
Donna Molaie
Kevin M. Tan
Rhusheet Patel
Manda V. Sasidhar
Source :
Brain Pathology. 23:462-475
Publication Year :
2013
Publisher :
Wiley, 2013.

Abstract

Sex differences in the structure and organization of the corpus callosum (CC) can be attributed to genetic, hormonal or environmental effects, or a combination of these factors. To address the role of gonadal hormones on axon myelination, functional axon conduction and immunohistochemistry analysis of the CC in intact, gonadectomized and hormone-replaced gonadectomized animals were used. These groups were subjected to cuprizone diet-induced demyelination followed by remyelination. The myelinated component of callosal compound action potential was significantly decreased in ovariectomized and castrated animals under normal myelinating condition. Compared to gonadally intact cohorts, both gonadectomized groups displayed more severe demyelination and inhibited remyelination. Castration in males was more deleterious than ovariectomy in females. Callosal conduction in estradiol-supplemented ovariectomized females was significantly increased during normal myelination, less attenuated during demyelination, and increased beyond placebo-treated ovariectomized or intact female levels during remyelination. In castrated males, the non-aromatizing steroid dihydrotestosterone was less efficient than testosterone and estradiol in restoring normal myelination/axon conduction and remyelination to levels of intact males. Furthermore, in both sexes, estradiol supplementation in gonadectomized groups increased the number of oligodendrocytes. These studies suggest an essential role of estradiol to promote efficient CC myelination and axon conduction in both sexes.

Details

ISSN :
10156305
Volume :
23
Database :
OpenAIRE
Journal :
Brain Pathology
Accession number :
edsair.doi...........72cbf9b8a10f8621f5685a8e87405f79
Full Text :
https://doi.org/10.1111/bpa.12029