Dehydroepiandrosterone biosynthesis, role, and mechanism of action in the developing neural tube

Dehydroepiandrosterone (DHEA) is synthesized from cholesterol by activity of P450scc and P450c17, enzymes that we previously characterized in the developing nervous system. We describe the localization of P450c17 in the differentiated field of the ventral spinal cord in different motor neuron subtyp...

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Published inFrontiers in endocrinology (Lausanne) Vol. 3; p. 16
Main Authors Galdo, Mark, Gregonis, Jennifer, Fiore, Christelle S, Compagnone, Nathalie A
Format Journal Article
LanguageEnglish
Published Switzerland Frontiers Research Foundation 2012
Frontiers Media S.A
Subjects
Dehydroepiandrosterone
DHEA
Endocrinology
induction
neurosteroid
proliferation
Spinal Cord
DHEA
induction
proliferation
sonic hedgehog
neural precursors
spinal cord
neurosteroid
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Summary:Dehydroepiandrosterone (DHEA) is synthesized from cholesterol by activity of P450scc and P450c17, enzymes that we previously characterized in the developing nervous system. We describe the localization of P450c17 in the differentiated field of the ventral spinal cord in different motor neuron subtypes. We show that, during organogenesis, P450c17 activity is regulated along the antero/posterior axis of the spinal cord concomitantly with the gradient of neurogenesis. To examine whether DHEA may modulate this process, we measured proliferation and differentiation of ventral neural precursors in primary and explant cultures. Our results showed that DHEA-induced the expression of class II protein Nkx6.1, motor neuron precursor Olig-2, and definitive motor neuron marker Isl-1/2. DHEA also promoted proliferation of ventrally committed precursors in isolated spinal cord precursor cultures and in whole spinal cord explants. Both the proliferative and inductive effects of DHEA were dependent on sonic hedgehog signaling. The possibilities that the effects observed with DHEA were due to its metabolism into androgens or to activation of NMDA receptors were excluded. These results support the hypothesis that the tight regulation of DHEA biosynthesis may be a biologic clock restricting the period of ventral neuronal-precursor proliferation, thus controlling the number of pre-committed neurons in the developing neural tube.
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Edited by: Kazuyoshi Tsutsui, Waseda University, Japan
Reviewed by: Synthia H. Mellon, University of California San Francisco, USA; Ishwar Parhar, Monash University, Malaysia
This article was submitted to Frontiers in Neuroendocrine Science, a specialty of Frontiers in Endocrinology.
ISSN:1664-2392
1664-2392
DOI:10.3389/fendo.2012.00016