UMLS:C1835664 - FACTA Search

Gene/Protein Disease Symptom Drug Enzyme Compound
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Query: UMLS:C1835664 (TOC)
2,763 document(s) hit in 31,850,051 MEDLINE articles (0.00 seconds)

A novel water quality index, the mutagen formation potential (MFP) is proposed for use in evaluation of the quality of drinking water which may contain pollutants capable of forming mutagens when chlorinated under the conditions used in water purification processes. A method for measuring MFP was established as follows. The water sample to be tested is diluted until the TOC reaches 3-4 mg l-1, the pH is adjusted to 7.0 +/- 0.2, sodium hypochlorite is added to obtain conditions where Cl/TOC = 3-4 mg Cl (mg C)-1, and the water sample is left standing for 24 +/- 2 h at room temperature. Thereafter, 21 of the chlorinated water sample at pH 2.0 +/- 0.1 is passed through a Sep-Pak Plus CSP-800 cartridge to adsorb any mutagens formed, and DMSO is applied to the cartridge to desorb the mutagens. Then, a 2 ml sample of the eluate is collected after the DMSO had begun to flow out of the cartridge and evaluated by the Ames Salmonella mutagenicity assay (preincubation method).
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PMID:Method for measuring mutagen formation potential (MFP) on chlorination as a new water quality index. 1132 63

The complete mineralization of concentrated solutions of Diclofenac (2-[(2,6-dichlorophenyl) amino] benzene-acetic acid) sodium salt C14H10C12NO2Na was carried out in a concentric cylindrical immersion photoreactor in batch mode operation. Irradiation with a lamp emitting light at 254 nm (400 W) achieved total mineralization of Diclofenac solutions (0.062 mM or TOC 20 mg C l(-1)) in times under an hour. The mineralization was carried out via Fenton photo-assisted treatment. A determination of the solution parameters was carried out to optimize the time of the Diclofenac pretreatment, the type and intensity of the light source, the effect of the concentrations of Fe-ions and the oxidant added in solution and the reactor recirculation rate. Diclofenac disappearance was monitored by high liquid pressure chromatography (HPLC). Concomitantly, the aromatic and aliphatic intermediates were also monitored under low-energy (36 W) light irradiation at 366 nm in order to be able to detect the intermediates by HPLC in the minute time scale. The decrease of the chemical oxygen demand was followed during Diclofenac degradation. The activation energy for the mineralization of Diclofenac was determined to be 4.02 Kcal mol(-1).
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PMID:Accelerated mineralization of the drug Diclofenac via Fenton reactions in a concentric photo-reactor. 1223 Feb 1

One of the major problems encountered in the textile industry is production of highly colored large volumes of wastewater. It is often not possible to predict the characteristics of textile wastewaters by using reported values in the literature because every textile industry is unique with respect to the type of production and the technology and chemicals used in production. Furthermore, the concentrations of pollutants in textile wastewaters vary according to the wastewater management practices and amount of water used in the production. In the first part of this study, wastewater characteristics of a cotton mill textile industry were determined by using the normal and log-normal II distribution functions for flow, COD, TOC, pH and colour. These parameters were measured in the effluent of the equalization tank and the statistical fits were evaluated by using the chi-Square test. It was found that flow and TOC values fitted normal distribution; COD values fitted log-normal II distribution. On the other hand, pH and colour did not fit in to aforementioned distributions. In the second part of this study, the treatment of textile wastewater by coagulation/flocculation/precipitation (CFP) was investigated. Lime, iron and aluminum salts with anionic polielectrolite combination were used as coagulants. Aluminum salts and the combination FeSO4 + lime + polielectrolite were used to remove the colour from mixed textile wastewaters, successfully. On the other hand, FeSO4 + lime + polielectrolite was more effective than aluminum salts to remove the colour from wastewater of indigo dyeing process. In the third part of this work, the removal of sulfide arising from indigo dyeing was investigated. Sulfide removal was accomplished by chemical oxidation and catalyzed air oxidation and removal efficiencies up to ninety percent were found. Chemical oxidation using sodium hypochlorite resulted in color removal too; however, dosages of hypochlorite have to be carefully monitored in order to avoid toxic effects of excess chlorine in water.
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PMID:Chemical treatment of textile wastewaters: statistical characterization, colour and sulfide removal. 1239 14

There is an increasing demand for measurement of organic carbon in solutions both in industry and in environmental research for the purpose of continuous water-quality monitoring. Practically all the methods used are based on a catalytic system in which metal oxides play a major role. The development of a new TOC/DOC measurement system, in our work, uses a mixed anatase-rutile form of TiO(2 )as catalyst of the mineralisation process, and direct measurement of the CO(2) produced, by a gaseous diffusion electrode. The entire research is based on heterogeneous catalysis using an immobilised catalyst, which can offer considerable advantages over other methods of catalysis. Four different catalytic systems were analysed. Three involved thermal immobilisation of TiO(2) on glass supports (glass spheres and glassy particulates) or on an Al metal grid. One further system consisted of direct oxidation of a Ti grid at high temperatures. The system was illuminated using a 350 nm UV source (350 mW cm(-2)) contained in a home-made measurement cell. Five molecules-malic acid, pentachlorophenol, sodium dodecylsulfate, hydroquinone, and citric acid-which were deemed to be representative and had been investigated in several previous studies, were used as photodegradation targets. However, it was not possible to obtain a direct expression of "catalytic efficiency" simply by reading the data obtained, nor any indirect molecular "recalcitrancy" scale. Chemometric analysis, by principal components analysis, allows the five used catalytic systems to be easily compared each other and a single PC component is able to perform classification.
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PMID:Chemometric investigation of the efficiency of different TiO(2)-based catalysts as principal components of TOC photochemical sensors under development. 1274 55

[(99m)Tc-EDDA-HYNIC-D-Phe(1),Tyr(3)]-Octreotide ((99m)Tc-EDDA/HYNIC-TOC) is a promising new radiopharmaceutical with the potential to replace [(111)In-DTPA-D-Phe(1)]-Octreotide ((111)In-DTPA-OCT) as the radiopharmaceutical for somatostatin receptor scintigraphy due to the advantage of improved image quality, lower radiation dose for the patient, and daily availability. Here we describe the development of a freeze-dried kit formulation based on the Tricine/EDDA exchange labeling approach for the preparation of this radiopharmaceutical in a clinical setting. Three parameters were of major importance to achieve a suitable formulation with a radiochemical purity (RCP) >90%: addition of bulking agent, the pH of the freeze-drying solution, and the content of stannous chloride. The final formulation consisted of 20 mg Tricine, 10 mg EDDA, 50 mg Mannitol, 20 microg SnCl(2). 2H(2)O, and 20 microg [HYNIC-D-Phe(1), Tyr(3)]-Octreotide (HYNIC-TOC). Radiolabeling was performed by addition of 0.2 M Na(2)HPO(4) to adjust the pH to 6-7, followed by 0.5-2 GBq (99m)Tc sodium pertechnetate, in a total volume of 2 mL and incubation for 10 min in a boiling water bath. Mean RCP values of 10 batches showed values >90% over a storage period of up to 1 year, a high stability up to 24 h of the final preparation, and retained biological activity. The developed kit formulation forms the basis for further clinical evaluation of this promising new radiopharmaceutical.
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PMID:Radiopharmaceutical development of a freeze-dried kit formulation for the preparation of [99mTc-EDDA-HYNIC-D-Phe1, Tyr3]-octreotide, a somatostatin analog for tumor diagnosis. 1534 59

Interactions between sodium dodecyl sulfate and zein protein, a model system for the understanding of the effect of surfactants on skin, were investigated using a range of techniques involving UV-vis spectroscopy, TOC (total organic carbon analysis), electrophoresis, and static and dynamic light scattering. Zein protein was solubilized by SDS. The adsorption of SDS onto insoluble protein fraction caused the zeta potential of the complex to become more negative. From these values, we calculated the Gibbs energy of absorption, which decreases when the SDS concentration is raised. Finally the structure of the complex, based on the analysis by static and dynamic light scattering, is proposed to be rod like.
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PMID:Complexation between dodecyl sulfate surfactant and zein protein in solution. 1546 77

This research work investigated the physical and chemical properties of a new type of wastewater produced from the semiconductor industry. The wastewater generated from indium phosphide (InP) wafer backgrinding and sawing processes was characterized in term of its particle size distribution (PSD), zeta potential, suspended and dissolved solids, total organic carbon, and turbidity. The wastewater contained high concentration of fine InP dusts with a size ranging from 0.07 - 1.44 mm. In spite of its high concentration of suspended solids resulting in high turbidity up to 371 NTU, the wastewater contained very low organic matters (TOC < 2.2 mg l(-1)) and other inorganic impurities (SO4(2-) < 0.21 mg l(-1) and Na+ < 0.16 mg l(-1)). Based on the experimental data collected, the treatment technologies using chemical precipitation and ultrafiltration were applied to the wastewater. Both processes could effectively remove InP particles from the wastewater, however the coagulants in chemical precipitation introduced other ionic contents into the process resulting in difficulties of water recycling in the later stage. In comparison, ultrafiltration was more promising for InP wastewater treatment and recycling. Based on the results of this study, a full-scale UF system was built in a local semiconductor plant and it has successfully reclaimed water from the InP wastes for the past six months without any quality issue being raised.
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PMID:Characterization and ultrafiltration of semiconductor indium phosphide (InP) wastewater for recycling. 1574 6

Gateways to Clinical Trials is a guide to the most recent clinical trials in current literature and congresses. The data in the following tables have been retrieved from the Clinical Trials Knowledge Area of Prous Science Integrity, the drug discovery and development portal, http://integrity.prous.com. This issue focuses on the following selection of drugs: (-)-Epigallocatechin gallate, (Z)-4-hydroxytamoxifen; Ad.muIFN-beta AD-237, adalimumab, adefovir dipivoxil, agalsidase alfa, alemtuzumab, almotriptan, ALVAC vCP1452, alvimopan hydrate, ambrisentan, anakinra, anti-IFN-gamma MAb; Bimatoprost, BMS-188797, BMS-214662, bortezomib, bosentan, bovine lactoferrin; Caffeine, canertinib dihydrochloride, canfosfamide hydrochloride, cannabidiol, caspofungin acetate, cetuximab, cH36, ChimeriVax-JE, ciclesonide, cilansetron, cinacalcet hydrochloride, clopidogrel, CpG-7909, Cypher; Daptomycin, darbepoetin alfa, darifenacin hydrobromide, decitabine, denufosol tetrasodium, Dexamet, diindolemethane, drotrecogin alfa (activated), duloxetine hydrochloride, DX-9065a; E-7010, edaravone, efalizumab, eicosapentaenoic acid/docosahexaenoic acid, elacridar, eletriptan, emtricitabine, epratuzumab, erlotinib hydrochloride, ertapenem sodium, eszopiclone, everolimus, ezetimibe; Fludarabine, fondaparinux sodium; gamma-Hydroxybutyrate sodium, gavestinel sodium, gefitinib, granisetron-Biochronomer; Human Albumin, human insulin; Imatinib mesylate, indiplon, interleukin-2 XL, isatoribine, ISS-1018, i.v. gamma-globulin, ivabradine hydrochloride, ixabepilone; Lanthanum carbonate, L-arginine hydrochloride, liposomal doxorubicin, LY-450139; Magnesium sulfate, melatonin, motexafin gadolinium, mycophenolic acid sodium salt; Natalizumab, nesiritide, niacin/lovastatin; OGX-011, olmesartan medoxomil, omalizumab, ospemifene; PACAP38, panitumumab, parathyroid hormone (human recombinant), parecoxib sodium, patupilone, pegfilgrastim, peginterferon alfa-2a, peginterferon alfa-2b, peginterferon alfa-2b/ribavirin, pemetrexed disodium, pimecrolimus, pirfenidone, posaconazole, prasterone, pregabalin; R-112, ramelteon, ranolazine, rasagiline mesilate, rebimastat, roflumilast, rosuvastatin calcium, rotigotine hydrochloride, rupatadine fumarate; S-3013, S-3304, semustine, sitaxsentan sodium, St. John's Wort extract; Tadalafil, tamoxifen, Taxus, Tc-99m-EDDA-HYNIC-TOC, TH-9507, tiotropium bromide, tipifarnib, tocilizumab, tolvaptan, torcetrapib, TR-14035, tramadol hydrochloride/acetaminophen, treprostinil diethanolamine, troglitazone, troxacitabine; Valdecoxib, valganciclovir hydrochloride, vandetanib, vardenafil hydrochloride hydrate, VAS-991, veglin, vinflunine, voriconazole; White sweet potato extract; Ximelagatran.
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PMID:Gateways to clinical trials. 1627 37

Exposure to hexavalent chromium (Cr(6+)) causes mutagenic, carcinogenic, and toxic effects, some of which have been associated with its oxidative capacity. In the kidney, Cr(6+) has been claimed to provoke necrosis of the proximal tubular cells. Our aim was to assess the functional involvement of the different segments that form the nephron in a model of acute renal failure caused by potassium dichromate and the participation of oxidative damage in this process. We also studied the possible protective effect of alpha-tocopherol (alpha-TOC) against renal damage. Wistar female rats 200g body weight (bw) received potassium dichromate (15mg/kg, sc, single dose). Lipid peroxidation and renal function were evaluated on days 0, 1, 2, 3, 7, 10, and 14. A second group received alpha-TOC (125mg/kg, by gavage) 5 days before and during dichromate exposure (same dose as for the first group), and was monitored at 0, 2, and 7 days of exposure. Creatinine clearance, glucose and sodium fractional excretions, p-aminohippurate uptake, free-water and osmolal clearances were also measured. Thiobarbituric acid-reactive substances were quantified in renal cortex. The results revealed altered proximal tubule function, decreased glomerular filtration, and distal segment dysfunction, accompanied by oxidative damage 48h after exposure to dichromate. In the alpha-TOC-treated group proximal reabsorptive and secretory functions were preserved, suggesting that oxidative damage is a participating mechanism in dichromate toxicity on these functions. In contrast alpha-TOC did not prevent glomerular or distal dysfunction, indicating selectivity of the protection afforded by this compound on the toxicity of dichromate, at the several components of the nephron.
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PMID:Alpha-tocopherol protects against the renal damage caused by potassium dichromate. 1634 25

Inorganic arsenic (iAs) exposure causes peripheral neuropathy. Oxidative effects caused by iAs exposure in peripheral nerves have been incompletely characterized. This study analyzed arsenic and lipid oxidative damage in the brain, spinal cord, and sciatic and sensory sural nerves following arsenite exposure. This study also explored whether alpha tocopherol (alpha-TOC) administration mitigates arsenite-induced oxidative damage. Thiobarbituric acid-reactive substance (TBARS) levels and distributions of iAs and its metabolites were evaluated in male Wistar rats following 30d of sodium arsenite exposure (10mg/kg bodyweight (bw)/d, by gavage). A second group also received alpha-TOC (125mg/kg bw/d, by gavage) during the final 20d of arsenite administration. Arsenite exposure caused increased TBARS levels within each region of the nervous system; oxidative stress was most pronounced in the sural and sciatic nerves. In addition there was a positive quadratic relationship between TBARS levels and the concentration of arsenicals found in the nervous system (r(2)=0.878, p<0.001). Dimethylarsenic was the predominant metabolite of iAs found. Animals alpha-TOC-treated had a 1.7-5.2-fold reduction in TBARS levels when compared with rats that received iAs alone. These results suggest that oxidative damage may be the main mechanism of toxicity induced by exposure of the peripheral nervous system to arsenite and that such damage could be attenuated by alpha-TOC-supplementation.
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PMID:Lipid oxidative damage and distribution of inorganic arsenic and its metabolites in the rat nervous system after arsenite exposure: influence of alpha tocopherol supplementation. 1679 74

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