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Estrogen signaling in arcuate Kiss1 neurons suppresses a sex-dependent female circuit promoting dense strong bones.

Citation
Herber, C. B., et al. “Estrogen Signaling In Arcuate Kiss1 Neurons Suppresses A Sex-Dependent Female Circuit Promoting Dense Strong Bones.”. Nature Communications, p. 163.
Center Vanderbilt University
Multicenter
Multicenter
Author Candice B Herber, William C Krause, Liping Wang, James R Bayrer, Alfred Li, Matthew Schmitz, Aaron Fields, Breanna Ford, Zhi Zhang, Michelle S Reid, Daniel K Nomura, Robert A Nissenson, Stephanie M Correa, Holly A Ingraham
Abstract

Central estrogen signaling coordinates energy expenditure, reproduction, and in concert with peripheral estrogen impacts skeletal homeostasis in females. Here, we ablate estrogen receptor alpha (ERα) in the medial basal hypothalamus and find a robust bone phenotype only in female mice that results in exceptionally strong trabecular and cortical bones, whose density surpasses other reported mouse models. Stereotaxic guided deletion of ERα in the arcuate nucleus increases bone mass in intact and ovariectomized females, confirming the central role of estrogen signaling in this sex-dependent bone phenotype. Loss of ERα in kisspeptin (Kiss1)-expressing cells is sufficient to recapitulate the bone phenotype, identifying Kiss1 neurons as a critical node in this powerful neuroskeletal circuit. We propose that this newly-identified female brain-to-bone pathway exists as a homeostatic regulator diverting calcium and energy stores from bone building when energetic demands are high. Our work reveals a previously unknown target for treatment of age-related bone disease.

Year of Publication
2019
Journal
Nature communications
Volume
10
Issue
1
Number of Pages
163
Date Published
12/2019
ISSN Number
2041-1723
DOI
10.1038/s41467-018-08046-4
Alternate Journal
Nat Commun
PMID
30635563
PMCID
PMC6329772
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