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Publication : Estrogen-negative feedback and estrous cyclicity are critically dependent upon estrogen receptor-α expression in the arcuate nucleus of adult female mice.

First Author  Yeo SH Year  2014
Journal  Endocrinology Volume  155
Issue  8 Pages  2986-95
PubMed ID  24905671 Mgi Jnum  J:214453
Mgi Id  MGI:5603001 Doi  10.1210/en.2014-1128
Citation  Yeo SH, et al. (2014) Estrogen-negative feedback and estrous cyclicity are critically dependent upon estrogen receptor-alpha expression in the arcuate nucleus of adult female mice. Endocrinology 155(8):2986-95
abstractText  The location and characteristics of cells within the brain that suppress GnRH neuron activity to contribute to the estrogen-negative feedback mechanism are poorly understood. Using adeno-associated virus (AAV)-mediated Cre-LoxP recombination in estrogen receptor-alpha (ERalpha) floxed mice (ERalpha(flox/flox)), we aimed to examine the role of ERalpha-expressing neurons located in the arcuate nucleus (ARN) in the estrogen-negative feedback mechanism. Bilateral injection of AAV-Cre into the ARN of ERalpha(flox/flox) mice (n = 14) resulted in the time-dependent ablation of up to 99% of ERalpha-immunoreactive cell numbers throughout the rostrocaudal length of the ARN. These mice were all acyclic by 5 weeks after AAV-Cre injections with most mice in constant estrous. Control wild-type mice injected with AAV-Cre (n = 13) were normal. Body weight was not altered in ERalpha(flox/flox) mice. After ovariectomy, a significant increment in LH secretion was observed in all genotypes, although its magnitude was reduced in ERalpha(flox/flox) mice. Acute and chronic estrogen-negative feedback were assessed by administering 17beta-estradiol to mice as a bolus (LH measured 3 h later) or SILASTIC brand capsule implant (LH measured 5 d later). This demonstrated that chronic estrogen feedback was absent in ERalpha(flox/flox) mice, whereas the acute feedback was normal. These results reveal a critical role for ERalpha-expressing cells within the ARN in both estrous cyclicity and the chronic estrogen negative feedback mechanism in female mice. This suggests that ARN cells provide a key indirect, transsynpatic route through which estradiol suppresses the activity of GnRH neurons.
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