Pilar Pérez scite author profile

We tested some resin-based composites used in dentistry for their estrogenic activity. A sealant based on bisphenol-A diglycidylether methacrylate (bis-GMA) increased cell yields, progesterone receptor expression, and pS2 secretion in human estrogen-target, serum-sensitive MCF7 breast cancer cells. Estrogenicity was due to bisphenol-A and bisphenol-A dimethacrylate, monomers found in the base paste of the dental sealant and identified by mass spectrometry. Samples of saliva from 18 subjects treated with 50 mg of a bis-GMA-based sealant applied on their molars were collected 1 hr before and after treatment. Bisphenol-A (range 90-931 micrograms) was identified only in saliva collected during a 1-hr period after treatment. The use of bis-GMA-based resins in dentistry, and particularly the use of sealants in children, appears to contribute to human exposure to xenoestrogens.ImagesFigure 1. AFigure 1. BFigure 2.Figure 3. AFigure 3. BFigure 4. AFigure 4. BFigure 5. AFigure 5. BFigure 6. AFigure 6. BFigure 7. AFigure 7. BFigure 8.Figure 9.Figure 10.

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Comparison of Short-Term Estrogenicity Tests for Identification of Hormone-Disrupting Chemicals

Andersen¹,

Andersson

Arnold

et al. 1999

Environ Health Perspect

396

163

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A comparison between two brine shrimp assays to detect in vitrocytotoxicity in marine natural products

Carballo¹,

Hernández-Inda²,

Pérez³

et al. 2002

BMC Biotechnol

283

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Background: The brine shrimp lethality assay is considered a useful tool for preliminary assessment of toxicity. It has also been suggested for screening pharmacological activities in plant extracts. However, we think that it is necessary to evaluate the suitability of the brine shrimp methods before they are used as a general bio-assay to test natural marine products for pharmacological activity.

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The estrogenicity of bisphenol A-related diphenylalkanes with various substituents at the central carbon and the hydroxy groups.

Pérez

Pulgar

Olea‐Serrano

et al. 1998

Environ Health Perspect

234

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The chemical structure of hydroxylated diphenylalkanes or bisphenols consists of two phenolic rings joined together through a bridging carbon. This class of endocrine disruptors that mimic estrogens is widely used in industry, particularly in plastics. Bisphenol F, bisphenol A, fluorine-containing bisphenol A (bisphenol AF), and other diphenylalkanes were found to be estrogenic in a bioassay with MCF7 human breast cancer cells in culture (E-SCREEN assay). Bisphenols promoted cell proliferation and increased the synthesis and secretion of cell type-specific proteins. When ranked by proliferative potency, the longer the alkyl substituent at the bridging carbon, the lower the concentration needed for maximal cell yield; the most active compound contained two propyl chains at the bridging carbon. Bisphenols with two hydroxyl groups in the para position and an angular configuration are suitable for appropriate hydrogen bonding to the acceptor site of the estrogen receptor. Our data suggest that estrogenicity is influenced not only by the length of the substituents at the bridging carbon but also by their nature. Because diphenylalkane derivatives are widespread and their production and use are increasing, potential exposure of humans to estrogenic bisphenols is becoming a significant issue. The hazardous effects of inadvertent exposure to bisphenol-releasing chemicals in professional workers and the general populations therefore deserve investigation.ImagesFigure 1Figure 2Figure 3Figure 4

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Treatment of advanced prostatic carcinoma with D-Trp-6-LH-RH

Bárcena¹,

Pérez²,

Ureta³

et al. 1984

Journal of Steroid Biochemistry

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Pilar Pérez

Estrogenicity of resin-based composites and sealants used in dentistry.

Comparison of Short-Term Estrogenicity Tests for Identification of Hormone-Disrupting Chemicals

A comparison between two brine shrimp assays to detect in vitrocytotoxicity in marine natural products

The estrogenicity of bisphenol A-related diphenylalkanes with various substituents at the central carbon and the hydroxy groups.

Treatment of advanced prostatic carcinoma with D-Trp-6-LH-RH

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