Estrogen protects against intracranial aneurysm rupture in ovariectomized mice

Authors

Yoshiteru Tada, University of California, San Francisco
Kosuke Wada, University of California, San Francisco
Kenji Shimada, University of California, San Francisco
Hiroshi Makino, University of California, San Francisco
Elena I. Liang, University of California, San Francisco
Shoko Murakami, University of California, San Francisco
Mari Kudo, University of California, San Francisco
Fumiaki Shikata, University of California, San Francisco
Ricardo A.Pena Silva, University of Iowa
Keiko T. Kitazato, Tokushima University Faculty of Medicine
David M. Hasan, University of Iowa
Yasuhisa Kanematsu, Tokushima University Faculty of Medicine
Shinji Nagahiro, Tokushima University Faculty of Medicine
Tomoki Hashimoto, University of California, San FranciscoFollow

Document Type

Article

Abstract

Clinical observations suggest that postmenopausal women have a higher incidence of aneurysmal rupture than premenopausal women. We hypothesize that a relative deficiency in estrogen may increase the risks of aneurysmal growth and subarachnoid hemorrhage in postmenopausal women. We assessed the effects of estrogen and selective estrogen receptor subtype agonists on the development of aneurysmal rupture in ovariectomized female mice. We used an intracranial aneurysm mouse model that recapitulates the key features of human intracranial aneurysms, including spontaneous rupture. Ten- to 12-week-old ovariectomized female mice received treatment with estrogen, nonselective estrogen receptor antagonist, estrogen receptor-α agonist, or estrogen receptor-β agonist starting 6 days after aneurysm induction so that the treatments affected the development of aneurysmal rupture without affecting aneurysmal formation. Estrogen significantly reduced the incidence of ruptured aneurysms and rupture rates in ovariectomized mice. Nonselective estrogen receptor antagonist abolished the protective effect of estrogen. Although estrogen receptor-α agonist did not affect the incidence of ruptured aneurysms or rupture rates, estrogen receptor-β agonist prevented aneurysmal rupture without affecting the formation of aneurysms. The protective role of estrogen receptor-β agonist was abolished by the inhibition of nitric oxide synthase. We showed that estrogen prevented aneurysmal rupture in ovariectomized female mice. The protective effect of estrogen seemed to occur through the activation of estrogen receptor-β, a predominant subtype of estrogen receptor in human intracranial aneurysms and cerebral arteries. © 2014 American Heart Association, Inc.

Keywords

Estrogens, Menopause, Models, animal

Publication Date

1-1-2014

Publication Title

Hypertension

ISSN

0194911X

E-ISSN

15244563

Volume

63

Issue

6

First Page

1339

Last Page

1344

PubMed ID

24732889

Digital Object Identifier (DOI)

10.1161/HYPERTENSIONAHA.114.03300

Recommended Citation

Tada, Yoshiteru; Wada, Kosuke; Shimada, Kenji; Makino, Hiroshi; Liang, Elena I.; Murakami, Shoko; Kudo, Mari; Shikata, Fumiaki; Silva, Ricardo A.Pena; Kitazato, Keiko T.; Hasan, David M.; Kanematsu, Yasuhisa; Nagahiro, Shinji; and Hashimoto, Tomoki, "Estrogen protects against intracranial aneurysm rupture in ovariectomized mice" (2014). Translational Neuroscience. 1671.
https://scholar.barrowneuro.org/neurobiology/1671