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In humans, early cortisol biosynthesis provides a mechanism to safeguard female sexual development

In humans, early cortisol biosynthesis provides a mechanism to safeguard female sexual development
In humans, early cortisol biosynthesis provides a mechanism to safeguard female sexual development
In humans, sexual differentiation of the external genitalia is established at 7–12 weeks post conception (wpc). During this period, maintaining the appropriate intrauterine hormone environment is critical. In contrast to other species, this regulation extends to the human fetal adrenal cortex, as evidenced by the virilization that is associated with various forms of congenital adrenal hyperplasia. The mechanism underlying these clinical findings has remained elusive. Here we show that the human fetal adrenal cortex synthesized cortisol much earlier than previously documented, an effect associated with transient expression of the orphan nuclear receptor nerve growth factor IB-like (NGFI-B) and its regulatory target, the steroidogenic enzyme type 2 3ß-hydroxysteroid dehydrogenase (HSD3B2). This cortisol biosynthesis was maximal at 8–9 wpc under the regulation of ACTH. Negative feedback was apparent at the anterior pituitary corticotrophs. ACTH also stimulated the adrenal gland to secrete androstenedione and testosterone. In concert, these data promote a distinctive mechanism for normal human development whereby cortisol production, determined by transient NGFI-B and HSD3B2 expression, provides feedback at the anterior pituitary to modulate androgen biosynthesis and safeguard normal female sexual differentiation.
0021-9738
953-960
Goto, Masahiro
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Piper Hanley, Karen Piper
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Marcos, Josep
df622d03-a354-4b44-8932-e46e15aa30d3
Wood, Peter J.
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Wright, Sarah
775184e7-df20-4253-86c9-90d25e2b104c
Postle, Anthony D.
0fa17988-b4a0-4cdc-819a-9ae15c5dad66
Cameron, Iain T.
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Mason, J. Ian
e771d06c-f850-430b-a34b-116bbccce3ec
Wilson, David I.
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Hanley, Neil A.
bf03f7bb-f377-44fb-8344-0bb1ca8b2ef9
Goto, Masahiro
5d3863d2-0efe-432b-a149-7cf53f5c1f58
Piper Hanley, Karen Piper
8b45e4d0-3fee-464d-9dc6-45630bfe5584
Marcos, Josep
df622d03-a354-4b44-8932-e46e15aa30d3
Wood, Peter J.
30039979-9541-4a0a-8aef-0dfe53114e02
Wright, Sarah
775184e7-df20-4253-86c9-90d25e2b104c
Postle, Anthony D.
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Cameron, Iain T.
f7595539-efa6-4687-b161-e1e93ff710f2
Mason, J. Ian
e771d06c-f850-430b-a34b-116bbccce3ec
Wilson, David I.
1500fca1-7082-4271-95f4-691f1d1252a2
Hanley, Neil A.
bf03f7bb-f377-44fb-8344-0bb1ca8b2ef9

Goto, Masahiro, Piper Hanley, Karen Piper, Marcos, Josep, Wood, Peter J., Wright, Sarah, Postle, Anthony D., Cameron, Iain T., Mason, J. Ian, Wilson, David I. and Hanley, Neil A. (2006) In humans, early cortisol biosynthesis provides a mechanism to safeguard female sexual development. Journal of Clinical Investigation, 116 (4), 953-960. (doi:10.1172/JCI25091).

Record type: Article

Abstract

In humans, sexual differentiation of the external genitalia is established at 7–12 weeks post conception (wpc). During this period, maintaining the appropriate intrauterine hormone environment is critical. In contrast to other species, this regulation extends to the human fetal adrenal cortex, as evidenced by the virilization that is associated with various forms of congenital adrenal hyperplasia. The mechanism underlying these clinical findings has remained elusive. Here we show that the human fetal adrenal cortex synthesized cortisol much earlier than previously documented, an effect associated with transient expression of the orphan nuclear receptor nerve growth factor IB-like (NGFI-B) and its regulatory target, the steroidogenic enzyme type 2 3ß-hydroxysteroid dehydrogenase (HSD3B2). This cortisol biosynthesis was maximal at 8–9 wpc under the regulation of ACTH. Negative feedback was apparent at the anterior pituitary corticotrophs. ACTH also stimulated the adrenal gland to secrete androstenedione and testosterone. In concert, these data promote a distinctive mechanism for normal human development whereby cortisol production, determined by transient NGFI-B and HSD3B2 expression, provides feedback at the anterior pituitary to modulate androgen biosynthesis and safeguard normal female sexual differentiation.

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Published date: 3 April 2006

Identifiers

Local EPrints ID: 27072
URI: http://eprints.soton.ac.uk/id/eprint/27072
ISSN: 0021-9738
PURE UUID: 487c95fa-68a8-45d6-b336-542e277ecbd3
ORCID for Anthony D. Postle: ORCID iD orcid.org/0000-0001-7361-0756
ORCID for Iain T. Cameron: ORCID iD orcid.org/0000-0002-4875-267X

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Date deposited: 25 Apr 2006
Last modified: 16 Mar 2024 03:00

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Contributors

Author: Masahiro Goto
Author: Karen Piper Piper Hanley
Author: Josep Marcos
Author: Peter J. Wood
Author: Sarah Wright
Author: Iain T. Cameron ORCID iD
Author: J. Ian Mason
Author: David I. Wilson
Author: Neil A. Hanley

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