Homology models of mouse and rat estrogen receptor-α ligand-binding domain created by in silico mutagenesis of a human template: Molecular docking with 17β-estradiol, diethylstilbestrol, and paraben analogs

Gonzalez, Thomas L.; Rae, James M.; Colacino, Justin A.; Richardson, Rudy J.

doi:10.1016/j.comtox.2018.11.003

Cited by 20 publications

(17 citation statements)

References 116 publications

(202 reference statements)

Supporting

Mentioning

Contrasting

Unclassified

Order By: Relevance

“…Differences in concentrations of methyl and propyl paraben biomarkers were among the highest observed in this study, particularly for the youngest non-Hispanic Black women. These chemicals have been used as preservatives in personal care products, pharmaceuticals, and food additives, and have been found to promote cell growth through multiple mechanisms, including estrogenicity (Gonzalez et al 2018, 2019; Okubo et al 2001) and epidermal growth factor receptor signaling (Pan et al 2016). Particularly relevant to our findings of the greatest methyl and ethyl paraben disparities in the youngest non-Hispanic Black women was the finding that early life paraben exposures can alter developing mammary gland morphology and induce gene expression that resembles an early cancer-like state (Gopalakrishnan et al 2017).…”

Section: Discussionmentioning

confidence: 99%

A comprehensive analysis of racial disparities in chemical biomarker concentrations in United States women, 1999-2014

Nguyen

Kahana

Heidt

et al. 2019

Preprint

Self Cite

View full text Add to dashboard Cite

27Background: Stark racial disparities in disease incidence among American women remains a persistent 28 public health challenge. These disparities likely result from complex interactions between genetic, social, 29 lifestyle, and environmental risk factors. The influence of environmental risk factors, such as chemical 30 exposure, however, may be substantial and is poorly understood. 31Objectives: We quantitatively evaluated chemical-exposure disparities by race/ethnicity and age in United 32 States (US) women by using biomarker data for 143 chemicals from the National Health and Nutrition 33 Examination Survey (NHANES) 1999(NHANES) -2014 Methods: We applied a series of survey-weighted, generalized linear models using data from the entire 35 NHANES women population and age-group stratified subpopulations. The outcome was chemical 36 biomarker concentration and the main predictor was race/ethnicity with adjustment for age, socioeconomic 37 status, smoking habits, and NHANES cycle. 38Results: The highest disparities across non-Hispanic Black, Mexican American, Other Hispanic, and other 39 race/multiracial women were observed for pesticides and their metabolites, including 2,5-dichlorophenol, 40 o,p'-DDE, beta-hexachlorocyclohexane, and 2,4-dichlorophenol, along with personal care and consumer 41 product compounds. The latter included parabens, monoethyl phthalate, and several metals, such as mercury 42 and arsenic. Moreover, for Mexican American, Other Hispanic, and non-Hispanic black women, there were 43 several exposure disparities that persisted across age groups, such as higher 2,4-and 2,5-dichlorophenol 44 concentrations. Exposure differences for methyl and propyl parabens, however, were the starkest between 45 non-Hispanic black and non-Hispanic white children with average differences exceeding 4 folds. 46 Discussions: We systematically evaluated differences in chemical exposures across women of various 47 race/ethnic groups and across age groups. Our findings could help inform chemical prioritization in 48 designing epidemiological and toxicological studies. In addition, they could help guide public health 49 interventions to reduce environmental and health disparities across populations.50 51 52The stark racial disparities in disease incidence and health outcomes among American women 53 remains a persistent public health challenge. For example, preterm birth incidence was found to be 54 approximately 60% higher in non-Hispanic Black women relative to non-Hispanic white women (Culhane 55 and Goldenberg 2011). Non-Hispanic Black and Hispanic women are at increased risk of being diagnosed 56 with developing dysglycemia (Marcinkevage et al. 2013) and diabetes (Cowie et al. 2009), relative to non-57 Hispanic white women. Non-Hispanic Black women are also 2-3 times more likely to develop the most 58 aggressive subtype of breast cancer, triple negative, compared to non-Hispanic white women (Carey et al. 59 2006; Stark et al. 2010). Furthermore, relative to non-Hispanic white women, non-Hispanic Black women...

show abstract

Section: Discussionmentioning

confidence: 99%

A comprehensive analysis of racial disparities in chemical biomarker concentrations in United States women, 1999-2014

Nguyen

Kahana

Heidt

et al. 2019

Preprint

Self Cite

View full text Add to dashboard Cite

show abstract

“…There are numerous affected signaling pathways after ED exposure in the animals. ERs and TRs are considered conservative receptors-for instance, in the case of ERα, ligand-binding affinity shows a distinct similarity between species [104,105]-however, the cellular composition can differ between rodents. Not only the specific "route of action"-the amounts of innate enzymes or receptors and specific enzyme isoforms-can be different between species, but the overall metabolic activity of the animals or the pace of development can vary between mice and rats as well.…”

Section: Discussionmentioning

confidence: 99%

Endocrine Disruptors Induced Distinct Expression of Thyroid and Estrogen Receptors in Rat versus Mouse Primary Cerebellar Cell Cultures

et al. 2019

View full text Add to dashboard Cite

The endocrine system of animals consists of fine-tuned self-regulating mechanisms that maintain the hormonal and neuronal milieu during tissue development. This complex system can be influenced by endocrine disruptors (ED)—substances that can alter the hormonal regulation even in small concentrations. By now, thousands of substances—either synthesized by the plastic, cosmetic, agricultural, or medical industry or occurring naturally in plants or in polluted groundwater—can act as EDs. Their identification and testing has been a hard-to-solve problem; Recent indications that the ED effects may be species-specific just further complicated the determination of biological ED effects. Here we compare the effects of bisphenol-A, zearalenone, and arsenic (well-known EDs) exerted on mouse and rat neural cell cultures by measuring the differences of the ED-affected neural estrogen- and thyroid receptors. EDs alters the receptor expression in a species-like manner detectable in the magnitude as well as in the nature of biological responses. It is concluded that the interspecies differences (or species specificity) in ED effects should be considered in the future testing of ED effects.

show abstract

“…DES is an analogue of the endogenous female sex hormone 17β-estradiol (E2) and binds to both the estrogen receptor α (ERα) and estrogen receptor β (ERβ) (Bolger et al 1998;Nikov et al 2001). It has been reported that the molecular dimensions of DES are almost identical to those of E2, particularly with regard to the distance between the terminal hydroxyl groups (Gonzalez et al 2019) (Fig. 1).…”

Section: Introductionmentioning

confidence: 59%

“…DES is an analogue of E2 and binds to both ERα and ERβ with a higher affinity compared to E2 Bolger et al 1998;Nikov et al 2001). It has been reported that the molecular dimensions of DES are almost identical to those of E2 (see figure 3), particularly with regard to the distance between the terminal hydroxyl groups (Gonzalez et al 2019). The length and breadth of both the steroid skeleton and the DES skeleton were shown to fit well into the receptorbinding pocket (Gonzalez et al 2019).…”

Section: Des and Breast Cancermentioning

confidence: 77%

“…Molecular docking of E2 and DES into the ligand binding domain of ERα from mouse and rat revealed similar binding orientations and confirmed a role for the hydroxyl moieties in this interaction (Gonzalez et al 2019). The ERα agonist action has generally been associated with stimulation of cell proliferation while ERβ activation has been linked with suppression of cell proliferation and stimulation of apoptosis (Sotoca et al 2008;Thomas and Gustafsson 2011).…”

Section: Introductionmentioning

confidence: 87%

See 1 more Smart Citation

Studying the role of estrogen receptor alpha in the developmental toxicity of diethylstilbestrol using alternative testing strategies

Adam¹

View full text Add to dashboard Cite

Table of Contents Chapter 1 General Introduction Chapter 2 Estrogen receptor alpha (ERα)-mediated coregulator binding and gene expression discriminates the toxic ERα agonist diethylstilbestrol (DES) from the endogenous ERα agonist 17β-estradiol (E2) Chapter 3 The in vivo developmental toxicity of diethylstilbestrol (DES) in rat evaluated by an alternative testing strategy Chapter 4 Assessment of the in vitro developmental toxicity of diethylstilbestrol and estradiol in the zebrafish embryotoxicity test Chapter 5 Physiologically based kinetic modelling-facilitated comparison of internal female dose levels of diethylstilbestrol and 17βestradiol, to study a potential role of kinetics in the differences in their developmental toxicity Chapter 6 General Discussion

show abstract

Homology models of mouse and rat estrogen receptor-α ligand-binding domain created by in silico mutagenesis of a human template: Molecular docking with 17β-estradiol, diethylstilbestrol, and paraben analogs

Cited by 20 publications

References 116 publications

A comprehensive analysis of racial disparities in chemical biomarker concentrations in United States women, 1999-2014

A comprehensive analysis of racial disparities in chemical biomarker concentrations in United States women, 1999-2014

Endocrine Disruptors Induced Distinct Expression of Thyroid and Estrogen Receptors in Rat versus Mouse Primary Cerebellar Cell Cultures

Studying the role of estrogen receptor alpha in the developmental toxicity of diethylstilbestrol using alternative testing strategies

Contact Info

Product

Resources

About