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Journal ArticleDOI

Antiestrogenicity of clarified slurry oil and two crude oils in a human breast-cancer cell assay.

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TLDR
The antiestrogenicity of the oil samples may occur through at least two mechanisms, increased catabolism of E2 and antagonistic binding to ER, as suggested by results from a whole-cell estrogen-receptor (ER) binding assay.
Abstract
Exposure to crude oil and certain petroleum products can be a serious health hazard. Clarified slurry oil (CSO) is a complex mixture of hydrocarbons derived from the process-ing of crude oil, and is a known systemic and developmental toxicant, mutagen, and carcinogen. In the present study, CSO and two crude oils, Belridge heavy crude oil (BHCO) and Lost Hills light crude oil (LHLCO), were examined for their estrogenic and antiestrogenic properties in a human breast-cancer cell (MCF-7) assay. The MCF-7 focus assay is based on postconfluent cell growth and tissue restructuring, measured as the postconfluent development of multicellular nodules or foci. The mutagenicity indices of BHCO and LHLCO also were determined in a modified Ames Salmonella assay. Oil samples were prepared in dimethyl sulfoxide, resulting in extraction of virtually all of the aromatic compounds including the sulfur- and nitrogen-substituted three- to seven-ring polycyclic aromatic compounds comprising 62.2% of the CSO, 9% of the BHCO, and 2% of the LHLCO by total weight. None of the three samples was estrogenic in the MCF-7 focus assay. In contrast, all of the samples were antiestrogenic; that is, they inbibited the development of foci induced by 1 nM 17β-estradiol (E 2 ). The potencies of the oil samples for both antiestrogenicity and mutagenicity were correlated with the percent of polycyclic aromatic compounds they contained. Two potential mechanisms for the observed antiestrogenicity were examined. Radiometric analysis of the catabolism of [ 3 H]E 2 in MCF-7 cell cultures demonstrated that all three samples increased catabolism of E 2 . Results from a whole-cell estrogen-receptor (ER) binding assay suggested that metabolites of compounds in the oil samples might have competed with [ 3 H]E 2 for ER in the MCF-7 cultures. Thus the antiestrogenicity of the oil samples may occur through at least two mechanisms, increased catabolism of E 2 and antagonistic binding to ER.

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Biomarkers of Exposure and Reproduction-Related Effects in Mussels Exposed to Endocrine Disruptors

TL;DR: The results confirm the usefulness of peroxisome proliferation as a biomarker of exposure to organic contaminants in mussels and indicate that changes in Vtg-like proteins could be used as potential indicator of pollutant effects on mussel reproduction.
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The generation, use and disposal of waste crankcase oil in developing countries: A case for Kampala district, Uganda

TL;DR: Lack of policy and information for proper handling of WCO contributed to the poor management of W CO exhibited and its disposal involved burning, and pouring in the environment.
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Systematic review of the association between oil and natural gas extraction processes and human reproduction

TL;DR: The results indicate there is moderate evidence for an increased risk of preterm birth, miscarriage, birth defects, decreased semen quality, and prostate cancer, and there is a negative impact on human reproduction from exposure to oil and gas activities.
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Unconventional oil and gas development and health outcomes: A scoping review of the epidemiological research.

TL;DR: A scoping review of epidemiological studies of exposure to unconventional oil and gas development found that 25 of the 29 studies reported at least one statistically significant association between the UOG exposure metric and an adverse health outcome.
References
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Book

The Chemistry and Technology of Petroleum

TL;DR: In this paper, Asphaltene used the data of the Data Structural Group Analysis (DSGAA) to determine the effect of various factors on the stability or instability of the Crude Oil System.
Journal ArticleDOI

17β-Estradiol hydroxylation catalyzed by human cytochrome P450 1A1: A comparison of the activities induced by 2,3,7,8-tetrachlorodibenzo-p-dioxin in MCF-7 cells with those from heterologous expression of the cDNA☆

TL;DR: Results provide strong evidence that P450 1A1 catalyzes the hydroxylations of E2 at the C-2, C-15 alpha, and C-6 alpha positions in incubations with microsomes from TCDD-treated MCF-7 cells, but suggest TCDd may also induce a cytochrome P450 E2 4-hydroxylase that is distinct from P450 2A1 or P 450 1A2.
Journal ArticleDOI

Molecular mechanism of inhibition of estrogen-induced cathepsin D gene expression by 2,3,7,8-tetrachlorodibenzo-p-dioxin (TCDD) in MCF-7 cells.

TL;DR: Electrophoretic mobility shift assays demonstrate that Ah receptor-mediated inhibition of E2-induced cathepsin D gene expression is due to disruption of the ER-Sp1 complex by targeted interaction with an overlapping XRE.
Journal ArticleDOI

Evidence of Estrogen- and TCDD-Like Activities in Crude and Fractionated Extracts of PM10 Air Particulate Material Using in Vitro Gene Expression Assays

TL;DR: Results from the analyses of nine environmentally prevalent polyaromatic hydrocarbons (PAH) indicated that PAH might be significant contributors to the observed activity.
Journal ArticleDOI

The effects of 2,3,7,8-tetrachlorodibenzo-p-dioxin on estrogen metabolism in MCF-7 breast cancer cells : evidence for induction of a novel 17β-estradiol 4-hydroxylase

TL;DR: Results provide additional evidence for the induction by TCDD of a novel E2 4-hydroxylase in MCF-7 cells but not in HepG2 cells and indicate possible endocrine regulatory roles for the newly discovered group of enzymes of the CYP1B subfamily.
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from a whole-cell estrogen-receptor (ER) binding assay suggested that metabolites of compounds in the oil samples might have competed with [3H]E2 for ER in the MCF-7 cultures.