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Institution

United States Environmental Protection Agency

GovernmentWashington D.C., District of Columbia, United States
About: United States Environmental Protection Agency is a government organization based out in Washington D.C., District of Columbia, United States. It is known for research contribution in the topics: Population & Environmental exposure. The organization has 13873 authors who have published 26902 publications receiving 1191729 citations. The organization is also known as: EPA & Environmental Protection Agency.


Papers
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Journal ArticleDOI
TL;DR: In this article, the degradation of polychlorinated biphenyls (PCBs) using sulfate radical-based advanced oxidation processes (SR-AOPs) was investigated.
Abstract: Polychlorinated biphenyls (PCBs) in the environment pose long-term risk to public health because of their persistent and toxic nature. This study investigates the degradation of PCBs using sulfate radical-based advanced oxidation processes (SR-AOPs). These processes are based on the generation of sulfate radicals through iron (Fe(II), Fe(III)) mediated activation of peroxymonosulfate (KHSO 5 , PMS) or persulfate (Na 2 S 2 O 8 , PS). This study is the first instance for coupling of Fe(II)/Fe(III) with PMS for PCB degradation in aqueous and sediment systems. The high oxidation efficiencies of the free radicals (SO 4 − ), in combination with the slow rate of consumption of the oxidants, make these processes very effective for the degradation of recalcitrant organic compounds. The effectiveness of the process was evaluated based on the degradation of a model polychlorinated biphenyl, 2-chlorobiphenyl and total organic carbon (TOC) removal. The kinetics of 2-chlorobiphenyl degradation along with the effect of oxidant and catalyst concentrations on the degradation efficiency was studied. Near complete removal of 2-chlorobiphenyl was observed when Fe(II) was used with PMS or PS. Fe(II) acts as a sulfate radical scavenger at higher concentrations indicating that there is an optimum concentration of Fe(II) that leads to most effective degradation of the target contaminant. A chelating agent, sodium citrate, was used to control the quantity of iron in the solution for activation of the oxidant. For the first time, we studied the feasibility of the activation of PMS using iron citrate complexes for PCB degradation. In the presence of sodium citrate, increase in degradation efficiency was observed up to a metal:ligand ratio of 1:2, after which the increase in citrate concentration led to a decrease in removal efficiency. Fe(II)/PMS systems were found to be very effective in degrading PCB in a sediment-slurry system with more than 90% PCB removal being observed within 24 h.

943 citations

Journal ArticleDOI
TL;DR: It is suggested that trivalent methylated arsenicals, intermediary products of arsenic methylation, may significantly contribute to the adverse effects associated with exposure to iAs, and high methylation capacity does not protect cells from the acute toxicity of triavalent arsenicals.
Abstract: Biomethylation is considered a major detoxification pathway for inorganic arsenicals (iAs). According to the postulated metabolic scheme, the methylation of iAs yields methylated metabolites in which arsenic is present in both pentavalent and trivalent forms. Pentavalent mono- and dimethylated arsenicals are less acutely toxic than iAs. However, little is known about the toxicity of trivalent methylated species. In the work reported here the toxicities of iAs and trivalent and pentavalent methylated arsenicals were examined in cultured human cells derived from tissues that are considered a major site for iAs methylation (liver) or targets for carcinogenic effects associated with exposure to iAs (skin, urinary bladder, and lung). To characterize the role of methylation in the protection against toxicity of arsenicals, the capacities of cells to produce methylated metabolites were also examined. In addition to human cells, primary rat hepatocytes were used as methylating controls. Among the arsenicals examined, trivalent monomethylated species were the most cytotoxic in all cell types. Trivalent dimethylated arsenicals were at least as cytotoxic as trivalent iAs (arsenite) for most cell types. Pentavalent arsenicals were significantly less cytotoxic than their trivalent analogs. Among the cell types examined, primary rat hepatocytes exhibited the greatest methylation capacity for iAs followed by primary human hepatocytes, epidermal keratinocytes, and bronchial epithelial cells. Cells derived from human bladder did not methylate iAs. There was no apparent correlation between susceptibility of cells to arsenic toxicity and their capacity to methylate iAs. These results suggest that (1) trivalent methylated arsenicals, intermediary products of arsenic methylation, may significantly contribute to the adverse effects associated with exposure to iAs, and (2) high methylation capacity does not protect cells from the acute toxicity of trivalent arsenicals.

934 citations

Journal ArticleDOI
10 Dec 2009-Nature
TL;DR: It is suggested that ecoenzymatic ratios reflect the equilibria between the elemental composition of microbial biomass and detrital organic matter and the efficiencies of microbial nutrient assimilation and growth.
Abstract: Biota can be described in terms of elemental composition, expressed as an atomic ratio of carbon:nitrogen:phosphorus (refs 1-3). The elemental stoichiometry of microoorganisms is fundamental for understanding the production dynamics and biogeochemical cycles of ecosystems because microbial biomass is the trophic base of detrital food webs. Here we show that heterotrophic microbial communities of diverse composition from terrestrial soils and freshwater sediments share a common functional stoichiometry in relation to organic nutrient acquisition. The activities of four enzymes that catalyse the hydrolysis of assimilable products from the principal environmental sources of C, N and P show similar scaling relationships over several orders of magnitude, with a mean ratio for C:N:P activities near 1:1:1 in all habitats. We suggest that these ecoenzymatic ratios reflect the equilibria between the elemental composition of microbial biomass and detrital organic matter and the efficiencies of microbial nutrient assimilation and growth. Because ecoenzymatic activities intersect the stoichiometric and metabolic theories of ecology, they provide a functional measure of the threshold at which control of community metabolism shifts from nutrient to energy flow.

917 citations

Journal ArticleDOI
TL;DR: Two QSAR models for developmental toxicity have been developed, using different statistical/mathematical methods, with the aim to minimize false negatives in order to make them more usable for REACH.
Abstract: The new REACH legislation requires assessment of a large number of chemicals in the European market for several endpoints. Developmental toxicity is one of the most difficult endpoints to assess, on account of the complexity, length and costs of experiments. Following the encouragement of QSAR (in silico) methods provided in the REACH itself, the CAESAR project has developed several models. Two QSAR models for developmental toxicity have been developed, using different statistical/mathematical methods. Both models performed well. The first makes a classification based on a random forest algorithm, while the second is based on an adaptive fuzzy partition algorithm. The first model has been implemented and inserted into the CAESAR on-line application, which is java-based software that allows everyone to freely use the models. The CAESAR QSAR models have been developed with the aim to minimize false negatives in order to make them more usable for REACH. The CAESAR on-line application ensures that both industry and regulators can easily access and use the developmental toxicity model (as well as the models for the other four endpoints).

913 citations


Authors

Showing all 13926 results

NameH-indexPapersCitations
Joel Schwartz1831149109985
Timothy A. Springer167669122421
Chien-Jen Chen12865566360
Matthew W. Gillman12652955835
J. D. Hansen12297576198
Dionysios D. Dionysiou11667548449
John P. Giesy114116262790
Douglas W. Dockery10524457461
Charles P. Gerba10269235871
David A. Savitz9957232947
Stephen Polasky9935459148
Judith C. Chow9642732632
Diane R. Gold9544330717
Scott L. Zeger9537778179
Rajender S. Varma9567237083
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Performance
Metrics
No. of papers from the Institution in previous years
YearPapers
202356
202279
2021780
2020787
2019852
2018929