Regulatory Role of G Protein–Coupled Estrogen Receptor for Vascular Function and Obesity

Haas, Elvira; Bhattacharya, Indranil; Brǎiloiu, Eugen; Damjanović, Marlen; Brailoiu, G. Cristina; Gào, Xīn; Mueller-Guerre, Laurence; Marjon, Nicole A.; Gut, A.; Minotti, Roberta; Meyer, Matthias R.; Amann, Kerstin; Ammann, Emerita; Perez-Dominguez, Ana; Genoni, Michele; Clegg, Deborah J.; Dun, Nae J.; Resta, Thomas C.; Prossnitz, Eric R.; Barton, Matthias

doi:10.1161/circresaha.108.190892

Cited by 330 publications

(466 citation statements)

References 18 publications

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“…in normal rats, the infusion of G-1 results in an acute reduction in mean arterial blood pressure within 2 min [30]. The effect of G-1 has been confirmed using GPR30 -/-mice.…”

Section: Circulatory Systemmentioning

confidence: 68%

“…The effect of G-1 has been confirmed using GPR30 -/-mice. The deletion of GPR30 from mice attenuates the G-1-induced relax of the carotid arteries, and there is no observed sex difference in the reductive effect of GPR30 [30]. The expression of the GPR30 mRNa is observed in the endothelium of the peripheral vessels of Lacz-introduced mice [19].…”

Section: Circulatory Systemmentioning

confidence: 94%

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In Vivo Functions of GPR30/GPER-1, a Membrane Receptor for Estrogen: From Discovery to Functions In Vivo

Mizukami

2010

Endocr J

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Summary. G protein-coupled receptor 30/G protein-coupled estrogen receptor-1 (GPR30/GPER-1) was reported as a novel membrane receptor for estrogen in 2005. However, the research on GPR30 has produced conflicting reports with regard to its intracellular localization, the tissue distribution of its expression, and some its functions. Recently, in addition to the finding of G-1, a GPR30 agonist, GPR30 KO mice have been produced in laboratories, and this has significantly increased the confidence in the data. In this review, the intrinsic appearance of GPR30 is approached based mainly on data obtained in vivo.

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“…in normal rats, the infusion of G-1 results in an acute reduction in mean arterial blood pressure within 2 min [30]. The effect of G-1 has been confirmed using GPR30 -/-mice.…”

Section: Circulatory Systemmentioning

confidence: 68%

Section: Circulatory Systemmentioning

confidence: 94%

In Vivo Functions of GPR30/GPER-1, a Membrane Receptor for Estrogen: From Discovery to Functions In Vivo

Mizukami

2010

Endocr J

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“…35 Role of the novel ER G protein coupled receptor 30 (GPR30) in the cardiovascular system In addition to the two classical ER subtypes, ERa and ERb, a third membrane-bound and G-protein-coupled ER, GPR30, has been identified in human vascular endothelial cells (ECs) and smooth muscle cells. [36][37][38] Haas et al 37 reported that G-1, a selective stimulator of GPR30, acutely blocked vasoconstrictor-induced changes in intracellular calcium concentrations and vascular tone, resulting in lowering of blood pressure in normotensive rats. Similar vasodilator effects of GPR30 have been confirmed in other studies.…”

Section: Action Of Estrogen On the Cardiovascular Systemmentioning

confidence: 99%

“…[39][40][41] It has also been reported that stimulation of GPR30 blocks VSMC proliferation. 37,42 The vasodilator action of G-1 may be mediated by NO-independent 40 and NO-dependent 37,39,40 pathways; the latter involves GPR30-induced endothelial NO synthase (eNOS) phosphorylation. 43 Also, G-1 decreases nicotinamide adenine dinucleotide phosphate-stimulated superoxide production by the carotid and intracranial arteries, indicating the scavenging effects of GPR30 on superoxide anions.…”

Section: Action Of Estrogen On the Cardiovascular Systemmentioning

confidence: 99%

Hormonal effects on blood vessels

Akishita

2012

Hypertens Res

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The incidence of cardiovascular disease (CVD) is lower in younger women than in men of the same age, but it increases after menopause, implicating the atheroprotective action of endogenous estrogen. Although observational studies have suggested the efficacy of estrogen therapy in postmenopausal women, placebo-controlled, randomized trials, such as the Women's Health Initiative, have not confirmed effects of estrogen therapy on CVD. Conversely, basic, experimental research has progressed and provided mechanistic insight into estrogen's action on blood vessels. By contrast, the vascular effects of androgens remain poorly understood and have been controversial for a long time. In recent years, an increasing body of evidence has suggested that androgens may exert protective effects against the development of atherosclerosis, at least in elderly men. Epidemiological studies have shown that the incidence of and mortality due to CVD were increased in elderly men with low testosterone levels, although the efficacy of androgen therapy remains unknown. Furthermore, recent experimental studies have demonstrated the direct action of androgens on the vasculature. In this review, we illustrate the effects of sex steroids on the cardiovascular system, focusing on the action of testosterone on the blood vessels.

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“…The effect of PMCA4b to promote GPER/ GPR30-mediated ERK1/2 phosphorylation likely plays a role in the initiation of more long term or genomic outcomes of GPER/ GPR30 activation. In addition, GPER/GPR30 agonist G-1 has been shown to acutely trigger Ca 2ϩ signals (50,51). In many cases, these Ca 2ϩ signals were used as a parameter of receptor activation (2,3,16).…”

mentioning

confidence: 99%

Hetero-oligomeric Complex between the G Protein-coupled Estrogen Receptor 1 and the Plasma Membrane Ca2+-ATPase 4b

Tran¹,

VerMeer²,

Burgard

et al. 2015

Journal of Biological Chemistry

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Regulatory Role of G Protein–Coupled Estrogen Receptor for Vascular Function and Obesity

Cited by 330 publications

References 18 publications

In Vivo Functions of GPR30/GPER-1, a Membrane Receptor for Estrogen: From Discovery to Functions In Vivo

In Vivo Functions of GPR30/GPER-1, a Membrane Receptor for Estrogen: From Discovery to Functions In Vivo

Hormonal effects on blood vessels

Hetero-oligomeric Complex between the G Protein-coupled Estrogen Receptor 1 and the Plasma Membrane Ca2+-ATPase 4b

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