Arsenic alters the function of the glucocorticoid receptor as a transcription factor.

Kaltreider, Ronald C.; Davis, Alisa M.; Lariviere, Jean P.; Hamilton, Joshua W.

doi:10.1289/ehp.01109245

Cited by 226 publications

(146 citation statements)

References 61 publications

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“…Environmental exposures may result in abnormal glucose metabolism, which in turn increases the risk of developing diabetes, through several plausible mechanisms (Longnecker and Daniels 2001). Arsenic is a known endocrine disruptor (Tseng 2004) and may disrupt the glucocorticoid receptor (Kaltreider et al 2001), which regulates a wide range of biological processes in humans, including insulin sensitivity. It is also possible that some aspect of having diabetes or prediabetes alters arsenic metabolism in such as way as to cause higher levels in the body.…”

Section: Discussionmentioning

confidence: 99%

Maternal Arsenic Exposure and Impaired Glucose Tolerance during Pregnancy

Ettinger¹,

Zota²,

Amarasiriwardena³

et al. 2009

Environ Health Perspect

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Section: Discussionmentioning

confidence: 99%

Maternal Arsenic Exposure and Impaired Glucose Tolerance during Pregnancy

Ettinger¹,

Zota²,

Amarasiriwardena³

et al. 2009

Environ Health Perspect

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“…H4IIE is a rat hepatoma cell line with 30,000-40,000 endogenous rGRs/cell. Culture of these lines was as described previously (10,16,18).…”

Section: Cell Lines and Vectorsmentioning

confidence: 99%

Arsenic Disruption of Steroid Receptor Gene Activation: Complex Dose−Response Effects Are Shared by Several Steroid Receptors

Bodwell¹,

Gosse

Nomikos

et al. 2006

Chem. Res. Toxicol.

111

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Chronic intake of arsenic (As) has been associated with increased risk of cancer, diabetes, developmental and reproductive problems, and cardiovascular disease. Recent studies suggest increased health risks with drinking water levels as low as 5-10 ppb. We previously reported that As disrupts glucocorticoid receptor (GR) mediated transcription in a very complex fashion. Low As levels (0.1 to 0.7 μM) stimulated transcription whereas slightly higher levels (1 to 3 μM) were inhibitory. The DNA Binding Domain (DBD) was the minimal region of GR required for the response to As. Mutations in the DBD that alter the conformation of the dimerization domain (D-Loop) to a DNA-bound GR conformation abolished the stimulatory effect and enhanced the inhibitory response to As. Here we report that receptors for progesterone (PR) and mineralocorticoids (MR) display a similar complex As response as the GR, suggesting a common mechanism for this effect. The complex response to As is not due to altered steroid or receptor levels. Moreover, a well-characterized GR dimerization mutant displayed a wild-type biphasic response to As for several divergent reporter genes, suggesting that dimerization is not critical for the response to As. Fluorescence polarization studies with purified PR and GR demonstrated that the specific PR/GR-DNA interaction is not altered in the presence of As. These results indicate that the numerous and diverse human health effects associated with As exposure maybe mediated, at least in part, through its ability to simultaneously disrupt multiple hormone receptor systems.

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“…Likewise, phagocytic activity of macrophages and other immune responses have been reported to be significantly reduced in arsenic-treated broiler chickens (Vodela et al 1997). Generally, arsenic can disrupt glucocorticoid regulation of immune function (Kaltreider et al 2001) and arsenic-mediated apoptosis may lead to a reduced/diminished immune response in mice (Harrison & McCoy 2001), rats (Bustamante et al 1997 (T-lymphocyte macrophage-dependent response) in rats exposed to arsenic. Arsenic trioxide treatment of mice caused suppressed primary humoral responses to SRBC (Burchiel et al 2009).…”

Section: Discussionmentioning

confidence: 99%

Immunosuppressive effects of arsenic in broiler chicks exposed to Newcastle disease virus

Sattar

Khan

Hussain

et al. 2016

Journal of Immunotoxicology

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To assess the effects of prolonged exposure to arsenic (As, as arsenate) on host immune competence overall and resistance to Newcastle disease (ND) viral infection in particular, a study was carried out in broiler chicks. At 7 days of age, chicks were assigned to groups that would undergo varying vaccination, challenge, and/or As exposures; Group 1 was a control; Group 2 was to receive Newcastle disease virus (NDV) only; two groups (Groups 3, 4) were to be given As daily (50 mg/kg, by gavage) from Days 7-35 of the experiment. All groups underwent normal vaccination on Days 5, 23, and 32 against live NDV (B1 type, LaSota strain); two groups (Groups 2, 4) were challenged with field-isolated NDV at Day 24. At Days 14, 21, 28, and 35 of age, subsets of chicks in each group were evaluated. The results showed feed intake and weight gain were lower in As-treated and NDV-challenged chicks. In As-treated chicks, absolute and relative spleen weights were significantly greater, whereas those of the thymus significantly lower, over the entire 35-day period. Effects on bursa weights (absolute, relative) were only significantly reduced through Day 21. Antibody titers against ND were significantly reduced (vs. control) over the whole 35 days in birds that received As alone, but only significantly depressed through the first 21 days in birds that received As þ NDV; thereafter, titers were significantly greater (in parallel with effects in birds that received NDV alone). In contrast, antibody responses to T-dependent antigen (Sheep red blood cells [SRBC]) were significantly lower in As only-and As þ NDV-treated chicks throughout the study period. Among birds exposed to As (alone or with NDV), in situ phagocytic activity was elevated and cutaneous sensitivity responses decreased during the period from Day 28 to Day 35. NDV alone had spurious effects on phagocytic activity but did cause significant reductions in cutaneous sensitivity responses. It was concluded that arsenic decreased immunity in broiler chicks, thereby making them prone to ND. ARTICLE HISTORY

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Arsenic alters the function of the glucocorticoid receptor as a transcription factor.

Cited by 226 publications

References 61 publications

Maternal Arsenic Exposure and Impaired Glucose Tolerance during Pregnancy

Maternal Arsenic Exposure and Impaired Glucose Tolerance during Pregnancy

Arsenic Disruption of Steroid Receptor Gene Activation: Complex Dose−Response Effects Are Shared by Several Steroid Receptors

Immunosuppressive effects of arsenic in broiler chicks exposed to Newcastle disease virus

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