Mutation of aspartic acid 262 on estrogen receptor abrogates estradiol signaling pathway

Autor:	Xingyan Xu, Haowei Yu, Shuihao Zhu, Ping Li, Xiaosa Li, Yongqi Gao, Yixiao Xiang, Guojun Zhao, Tommaso Simoncini, Huiping Lin
Jazyk:	angličtina
Rok vydání:	2023
Předmět:	Estrogen receptor nongenomic effects genomic actions vascular effects Gynecology and obstetrics RG1-991 Diseases of the endocrine glands. Clinical endocrinology RC648-665
Zdroj:	Gynecological Endocrinology, Vol 39, Iss 1 (2023)
Druh dokumentu:	article
ISSN:	09513590 1473-0766 0951-3590
DOI:	10.1080/09513590.2023.2250881
Popis:	Objective ERα (estrogen receptor alpha) exerts nuclear genomic actions and membrane-initiated non-genomic effects. The mutation of aspartic acid into alanine in vitro revealed the critical role of aspartic acid 258 (corresponding to mouse amino acid site 262) of ERα for non-nuclear function. Our previous in vitro study revealed that this mutation blocked estrogen’s non-genomic effects on vascular endothelial H2S release. Here, we studied the in vivo role of the aspartic acid 262 of ERα in the reproductive system and in the vascular tissue.Approach and Results We generated a mouse model harboring a point mutation of the murine counterpart of this aspartic acid into alanine (ERαD262A). Our results showed that the ERαD262A females are fertile with standard hormonal serum levels, but the uterine development and responded with estrogen and follicular development are disrupted. In line with our previous study, we found that the rapid dilation of the aorta was abrogated in ERαD262A mice. In contrast to the previously reported R264-ERα mice, the classical estrogen genomic effector SP1/NOS3/AP1 and the nongenomic effectors p-eNOs, p-AKT, and p-ERK were disturbed in the ERαD262A aorta. Besides, the serum H2S concentration was decreased in ERαD262A mice. Together, ERαD262A mice showed compromised both genomic and non-genomic actions in response to E2.Conclusions These data showed that aspartic acid 262 of ERα are important for both genomic and non-genomic effects of E2. Our data provide a theoretical basis for further selecting an effective non-genomic mouse model and provide a new direction for developing estrogen non-genomic effect inhibitors.
Databáze:	Directory of Open Access Journals
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