Abstract

Our previous studies suggest that prenatal arsenic exposure (50 ppb) modifies epigenetic control of the programming of the glucocorticoid receptor (GR) signaling system in the developing mouse brain. These deficits may lead to long-lasting consequences, including deficits in learning and memory, increased depressive-like behaviors, and an altered set-point of GR feedback throughout life. To understand the arsenic-induced changes within the GR system, we assessed the impact of in utero arsenic exposure on the levels of the GR and growth arrest-specific-5 (Gas5), a noncoding RNA, across a key gestational period for GR programming (gestational days, GD 14–18) in mice. Gas5 contains a glucocorticoid response element (GRE)-like sequence that binds the GR, thereby decreasing GR-GRE-dependent gene transcription and potentially altering GR programming. Prenatal arsenic exposure resulted in sex-dependent and age-dependent shifts in the levels of GR and Gas5 expression in fetal telencephalon. Nuclear GR levels were reduced in males, but unchanged in females, at all gestational time points tested. Total cellular Gas5 levels were lower in arsenic-exposed males with no changes seen in arsenic-exposed females at GD16 and 18. An increase in total cellular Gas-5 along with increased nuclear levels in GD14 arsenic-exposed females, suggests a differential regulation of cellular compartmentalization of Gas5. RIP assays revealed reduced Gas5 associated with the GR on GD14 in the nuclear fraction prepared from arsenic-exposed males and females. This decrease in levels of GR-Gas5 binding continued only in the females at GD18. Thus, nuclear GR signaling potential is decreased in prenatal arsenic-exposed males, while it is increased or maintained at levels approaching normal in prenatal arsenic-exposed females. These findings suggest that females, but not males, exposed to arsenic are able to regulate the levels of nuclear free GR by altering Gas5 levels, thereby keeping GR nuclear signaling closer to control (unexposed) levels.

Full Text
Published version (Free)

Talk to us

Join us for a 30 min session where you can share your feedback and ask us any queries you have

Schedule a call

Similar Papers

Paper Title
Journal
Date
Author
Arsenic exposure during embryonic development alters the expression of the long noncoding RNA growth arrest specific-5 (Gas5) in a sex-dependent manner
Alexander Hafez ... Andrea M Allan
Neurotoxicology and Teratology | VOL. 66
Alexander Hafez, et. al.Alexander Hafez ... Andrea M Allan
11 Nov 2017
Treatment of impaired wounds – Understanding the therapeutic mechanisms of umbilical cord-derived mesenchymal stem cells
A De La Fuente ... M Abal
Toxicology Letters | VOL. 295
A De La Fuente, et. al.A De La Fuente ... M Abal
12 Sep 2018
Sex-specific deficits in biochemical but not behavioral responses to delay fear conditioning in prenatal alcohol exposure mice.
Elizabeth R Solomon ... Andrea M Allan
Neurobiology of learning and memory | VOL. 156
Elizabeth R Solomon, et. al.Elizabeth R Solomon ... Andrea M Allan
12 Oct 2018
The role of glucocorticoid receptor phosphorylation in the model of negative affective states
Iva Lukic ... Marina Mihaljevic
The World Journal of Biological Psychiatry | VOL. 16
Iva Lukic, et. al.Iva Lukic ... Marina Mihaljevic
08 Mar 2015
View more papers

More From: Clinics in Chest Medicine

Paper Title
Journal
Date
Author
Contributors
-
Clinics in Chest Medicine | VOL. 45
--
01 Jun 2024
Copyright
-
Clinics in Chest Medicine | VOL. 45
--
01 Jun 2024
Contents
-
Clinics in Chest Medicine | VOL. 45
--
01 Jun 2024
Forthcoming Issues
-
Clinics in Chest Medicine | VOL. 45
--
01 Jun 2024
View more papers