17β‐Oestradiol Anti‐Inflammatory Effects in Primary Astrocytes Require Oestrogen Receptor β‐Mediated Neuroglobin Up‐Regulation

Marinis, Elisabetta De; Acaz‐Fonseca, Estefanía; Arévalo, María Ángeles; Ascenzi, Paolo; Fiocchetti, Marco; Marino, Maria; García‐Segura, Luis M.

doi:10.1111/jne.12007

Cited by 89 publications

(92 citation statements)

References 45 publications

Supporting

Mentioning

Contrasting

Unclassified

Order By: Relevance

“…For each steroid receptor, strongly coexpressed genes within a brain region are likely related to the localized functional role of the receptor. For example, of the top 10 genes coexpressed with Esr1 across the whole brain, four were previously shown to be regulated by ESR1 and/or estrogens in various tissues (Gpr101, Calcr, Ngb, and Gpx3) (12)(13)(14)(15). These genes were also coexpressed with Esr1 in the HY, in line with their functional relationship to Esr1 in mediating, for example, reproductive and metabolic processes.…”

Section: Genes Spatially Coexpressed With Steroid Receptors Indicate mentioning

confidence: 68%

Genome-wide coexpression of steroid receptors in the mouse brain: Identifying signaling pathways and functionally coordinated regions

Mahfouz

Lelieveldt

Grefhorst

et al. 2016

Proc. Natl. Acad. Sci. U.S.A.

View full text Add to dashboard Cite

Steroid receptors are pleiotropic transcription factors that coordinate adaptation to different physiological states. An important target organ is the brain, but even though their effects are well studied in specific regions, brain-wide steroid receptor targets and mediators remain largely unknown due to the complexity of the brain. Here, we tested the idea that novel aspects of steroid action can be identified through spatial correlation of steroid receptors with genome-wide mRNA expression across different regions in the mouse brain. First, we observed significant coexpression of six nuclear receptors (NRs) [androgen receptor (Ar), estrogen receptor alpha (Esr1), estrogen receptor beta (Esr2), glucocorticoid receptor (Gr), mineralocorticoid receptor (Mr), and progesterone receptor (Pgr)] with sets of steroid target genes that were identified in single brain regions. These coexpression relationships were also present in distinct other brain regions, suggestive of as yet unidentified coordinate regulation of brain regions by, for example, glucocorticoids and estrogens. Second, coexpression of a set of 62 known NR coregulators and the six steroid receptors in 12 nonoverlapping mouse brain regions revealed selective downstream pathways, such as Pak6 as a mediator for the effects of Ar and Gr on dopaminergic transmission. Third, Magel2 and Irs4 were identified and validated as strongly responsive targets to the estrogen diethylstilbestrol in the mouse hypothalamus. The brain-and genome-wide correlations of mRNA expression levels of six steroid receptors that we provide constitute a rich resource for further predictions and understanding of brain modulation by steroid hormones. neuroendocrinology | nuclear receptors | transcription regulation | estrogens | glucocorticoids S teroid receptors are part of the superfamily of nuclear receptors (NRs) that act as transcription factors regulating expression of numerous biologically important target genes (1). Their transcriptional activity is induced by steroid hormones, which respond to changed demands in terms of reproductive status, mineral balance, or stressful physical and psychological challenges. A crucial site of action is the brain, where these hormones have strong modulatory effects on physiological regulation, cognitive function, mood, and behavior. They do so by changing cellular responsiveness to a variety of neurotransmitters and peptides, and by inducing morphological changes (2, 3).Understanding the effects of steroid hormones on the brain faces the challenge to identify in as many as 900 different brain nuclei (4) both the highly cell-specific target genes that mediate the hormone effects (5, 6) and the signaling factors that mediate or influence steroid receptor signaling. The latter include proteins affecting prereceptor metabolism, interacting transcription factors (7), and downstream NR coregulator proteins (1). Even if the effects of steroid hormones are well-studied in specific regions (1, 8), overall, the brain steroid receptor targets and mediators ...

show abstract

Section: Genes Spatially Coexpressed With Steroid Receptors Indicate mentioning

confidence: 68%

Genome-wide coexpression of steroid receptors in the mouse brain: Identifying signaling pathways and functionally coordinated regions

Mahfouz

Lelieveldt

Grefhorst

et al. 2016

Proc. Natl. Acad. Sci. U.S.A.

View full text Add to dashboard Cite

show abstract

“…The current study demonstrated that 1-BP treatment decreased Ngb protein level in cerebral cortex in a dose-dependent manner. Ngb was expressed in neurons as well as astrocytes (De Marinis et al, 2013a, 2013b. Therefore, Ngb decrease induced by 1-BP made the cortical neurons more vulnerable to damage by reactive species and apoptosis which could cause neuron loss.…”

Section: Discussionmentioning

confidence: 97%

“…Ngb, firstly discovered in 2000, is expressed in neurons, astrocytes, retina and some endocrine tissues (Burmester et al, 2000;Burmester and Hankeln, 2004;De Marinis et al, 2013a). Brunori and Vallone (2007) demonstrated its highly conserved structure and function.…”

mentioning

confidence: 99%

Involvement of decreased neuroglobin protein level in cognitive dysfunction induced by 1-bromopropane in rats

Guo¹,

Yuan²,

Jiang³

et al. 2015

Brain Research

View full text Add to dashboard Cite

“…It has been reported that the two classic receptors for estrogen, estrogen receptor α (ERα), and estrogen receptor β (ERβ) are closely related with inflammation [11][12][13]. In contrast to the long association of ERα with pain, the association of ERβ with pain may have a totally contradictory role to that mediated by ERα [14][15][16].…”

Section: Introductionmentioning

confidence: 99%

Inhibitory effect of estrogen receptor beta on P2X3 receptors during inflammation in rats

Jiang

Sun

et al. 2016

Purinergic Signalling

View full text Add to dashboard Cite

Estrogen receptor beta (ERβ) has been shown to play a therapeutic role in inflammatory bowel disease (IBD). However, the mechanism underlying how ERβ exerts therapeutic effects and its relationship with P2X3 receptors (P2X3R) in rats with inflammation is not known. In our study, animal behavior tests, visceromotor reflex recording, and Western blotting were used to determine whether the therapeutic effect of ERβ in rats with inflammation was related with P2X3R. In complete Freund adjuvant (CFA)-induced chronic inflammation in rats, paw withdrawal threshold was significantly decreased which were then reversed by systemic injection of ERβ agonists, DPN or ERB-041. In 2,4,6-trinitrobenzene sulfonic acid (TNBS)-induced colitis in rats, weight loss, higher DAI scores, increased visceromotor responses, and inflammatory responses were reversed by application of DPN or ERB-041. The higher expressions of P2X3R in dorsal root ganglia (DRG) of CFA-treated rats and those in rectocolon and DRG of TNBS-treated rats were all decreased by injection of DPN or ERB-041. DPN application also inhibited P2X3R-evoked inward currents in DRG neurons from TNBS rats. Mechanical hyperalgesia and increased P2X3 expression in ovariectomized (OVX) CFA-treated rats were reversed by estrogen replacements. Furthermore, the expressions of extracellular signal-regulated kinase (ERK) in DRG and spinal cord dorsal horn (SCDH) and c-fos in SCDH were significantly decreased after estrogen replacement compared with those of OVX rats. The ERK antagonist U0126 significantly reversed mechanical hyperalgesia in the OVX rats. These results suggest that estrogen may play an important therapeutic role in inflammation through downregulation of P2X3R in peripheral tissues and the nervous system, probably via ERβ, suggesting a novel therapeutic strategy for clinical treatment of inflammation.

show abstract

17β‐Oestradiol Anti‐Inflammatory Effects in Primary Astrocytes Require Oestrogen Receptor β‐Mediated Neuroglobin Up‐Regulation

Cited by 89 publications

References 45 publications

Genome-wide coexpression of steroid receptors in the mouse brain: Identifying signaling pathways and functionally coordinated regions

Genome-wide coexpression of steroid receptors in the mouse brain: Identifying signaling pathways and functionally coordinated regions

Involvement of decreased neuroglobin protein level in cognitive dysfunction induced by 1-bromopropane in rats

Inhibitory effect of estrogen receptor beta on P2X3 receptors during inflammation in rats

Contact Info

Product

Resources

About