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      A multidisciplinary investigation of the technical and environmental performances of TAML/peroxide elimination of Bisphenol A compounds from water

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          Abstract

          A multidisciplinary investigation of the technical and environmental performances of TAML/peroxide elimination of Bisphenol A compounds from water: destruction, oligomerisation, mechanisms, end product toxicity, and applications.

          Abstract

          Designing technologies that mitigate the low-dose adverse effects of exposures to large-volume, everyday-everywhere chemicals such as bisphenol A (BPA, 1a) requires an understanding of the scope of the exposures and the nature of the adverse effects. Therefore, we review the literature of, (i) the occurrences of 1a in humans, waters and products and the effectiveness of widely deployed mitigation methods in 1a stewardship and, (ii) the adverse effects of 1a exposures on human cells and fish. Within this broad context, we present and evaluate experimental results on TAML/H 2O 2 purification of 1a contaminated waters. TAML/H 2O 2 catalysis readily oxidizes BPA ( 1a) and the ring-tetramethyl ( 1b), tetrachloro ( 1c), and tetrabromo ( 1d)-substituted derivatives. At pH 8.5, TAML/H 2O 2 induces controllable, oxidative oligomerisation of 1a (2-, 3-, 4-, and 5-unit species were identified) with precipitation, establishing a green synthetic pathway to these substances for biological safety characterisation and an easy method for near quantitative removal of 1a from water. TAML/H 2O 2 (24 nM/4 mM) treatment of 1a (10 000 μg L −1) in pH 8.5 (0.01 M, carbonate) lab water effects a >99% reduction (to <100 μg L −1 1a) within 30 min. Yeast oestrogen screens (YES) of the pH 8.5, TAML/H 2O 2 treated, catalase quenched, and filtered oxidation solutions show elimination of 1a oestrogenicity. Zebrafish developmental assays of TAML/H 2O 2 treated, unfiltered, agitated pH 7, 1a solutions showed no significant incidences of abnormality among any of 22 endpoints—treated samples showed an insignificant increase in mortality. At pH 11, the TAML/H 2O 2 oxidations of 1a–d are fast with second order rate constants for the substrate oxidation process ( k II values) of (0.57–8) × 10 4 M −1 s −1. The 1a oxidation gives CO and CO 2 (∼78%), acetone (∼25%) and formate (∼1%). In striking contrast with pH 8.5 treatment, no oligomers were detected. TAML/H 2O 2 (150 nM/7.5 mM) treatment of 1a (34 244 μg L −1) in pH 11 (0.01 M, phosphate) lab water effected a >99.9% reduction (to <23 μg L −1 1a) within 15 min. The pH dependent behaviour of 1a was examined as a possible origin of the differing outcomes. The 1 st and 2 nd p K a values of 1a were estimated by fitting the pH dependence of the UV-vis spectra (p K a1 = 9.4 ± 0.3; p K a2 = 10.37 ± 0.07). At pH 8.5, coupling of the radical produced on initial oxidation evidently outcompetes further oxidation. A linear free energy relationship between the logarithm of the pH 11, k II values and the redox potentials of 1a–d as determined by differential pulse voltammetry in CH 3CN is consistent with rate-limiting, electron transfer from the dianionic form of 1a at pH 11, followed by a multistep, deep degradation without observation of 4-(prop-1-en-2-yl)phenol 12, a common 1a oxidation product—an improved synthesis of 12 is described. Microtox® analyses of pH 12, TAML/H 2O 2 treated 1a solutions showed significantly reduced toxicity. The facility and high efficiency by which TAML/H 2O 2 catalysis eliminates 1a from water, by either mechanism, suggests a new and simple procedure for 1a stewardship.

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          Pharmaceuticals, Hormones, and Other Organic Wastewater Contaminants in U.S. Streams, 1999−2000:  A National Reconnaissance

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            Bisphenol A and human health: a review of the literature.

            There is growing evidence that bisphenol A (BPA) may adversely affect humans. BPA is an endocrine disruptor that has been shown to be harmful in laboratory animal studies. Until recently, there were relatively few epidemiological studies examining the relationship between BPA and health effects in humans. However, in the last year, the number of these studies has more than doubled. A comprehensive literature search found 91 studies linking BPA to human health; 53 published within the last year. This review outlines this body of literature, showing associations between BPA exposure and adverse perinatal, childhood, and adult health outcomes, including reproductive and developmental effects, metabolic disease, and other health effects. These studies encompass both prenatal and postnatal exposures, and include several study designs and population types. While it is difficult to make causal links with epidemiological studies, the growing human literature correlating environmental BPA exposure to adverse effects in humans, along with laboratory studies in many species including primates, provides increasing support that environmental BPA exposure can be harmful to humans, especially in regards to behavioral and other effects in children. Copyright © 2013 Elsevier Inc. All rights reserved.
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              In vivo effects of bisphenol A in laboratory rodent studies.

              Concern is mounting regarding the human health and environmental effects of bisphenol A (BPA), a high-production-volume chemical used in synthesis of plastics. We have reviewed the growing literature on effects of low doses of BPA, below 50 mg/(kg day), in laboratory exposures with mammalian model organisms. Many, but not all, effects of BPA are similar to effects seen in response to the model estrogens diethylstilbestrol and ethinylestradiol. For most effects, the potency of BPA is approximately 10-1000-fold less than that of diethylstilbestrol or ethinylestradiol. Based on our review of the literature, a consensus was reached regarding our level of confidence that particular outcomes occur in response to low dose BPA exposure. We are confident that adult exposure to BPA affects the male reproductive tract, and that long lasting, organizational effects in response to developmental exposure to BPA occur in the brain, the male reproductive system, and metabolic processes. We consider it likely, but requiring further confirmation, that adult exposure to BPA affects the brain, the female reproductive system, and the immune system, and that developmental effects occur in the female reproductive system.
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                Author and article information

                Journal
                GRCHFJ
                Green Chemistry
                Green Chem.
                Royal Society of Chemistry (RSC)
                1463-9262
                1463-9270
                2017
                2017
                : 19
                : 18
                : 4234-4262
                Article
                10.1039/C7GC01415E
                484d35cd-bf3b-434c-a1d2-1fd2d3f27bf6
                © 2017
                History

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