Your search keyword '"In vitro toxicity"' showing total 596 results

201. Polyphasic toxicological screening of Cylindrospermopsis raciborskii and Aphanizomenon gracile isolated in Poland

Author

Tomasz Jurczak, Piotr Rzymski, Miquel Lürling, Joanna Mankiewicz-Boczek, Mikołaj Kokociński, Barbara Poniedziałek, Ilona Gągała-Borowska, Andreas Ballot, and Elisabeth J. Faassen

Subjects

Environmental Risk Assessment, 0301 basic medicine, Aquatic Ecology and Water Quality Management, α-γ,-Diaminobutyric acid, Cyanotoxins, Metabolite, Microcystin, 010501 environmental sciences, medicine.disease_cause, 01 natural sciences, Cylindrospermopsis raciborskii, Microbiology, 03 medical and health sciences, chemistry.chemical_compound, Botany, medicine, α-γ, 0105 earth and related environmental sciences, Saxitoxin, Nostocales, chemistry.chemical_classification, WIMEK, biology, Toxin, Aphanizomenon gracile, Diaminobutyric acid, Aquatische Ecologie en Waterkwaliteitsbeheer, In vitro toxicity, biology.organism_classification, 030104 developmental biology, chemistry, Toxicity, Cylindrospermopsin, Agronomy and Crop Science

Abstract

Aphanizomenon gracile and Cylindrospermopsis raciborskii are extensively studied Nostocales of wide geographical distribution and have potential to produce toxins. However, a number of knowledge gaps regarding their toxicity and related health risks in certain locations, including Europe, exists. The present study applied a polyphasic approach to screen the toxicity of different strains of C. raciborskii (LBY-Cr, LBO-Cr and LKM-Cr) and A. gracile (LBY-Ag, LBN-Ag and LWI-Ag) isolated from five freshwater lakes of Western Poland. The following investigations were carried out: (i) in vitro toxicological studies employing human cells isolated from healthy donors; (ii) analytical screening for the presence of cylindrospermopsin (CYN), guanidinoacetate (GAA; initial CYN precursor and postulated general cyanobacterial metabolite), three microcystin (MC) analogues, β- N -methylamino- l -alanine (BMAA) and its isomer α-γ,-diaminobutyric acid (DAB), anatoxin-a (ATX) and ten saxitoxin (STX) analogues; and (iii) molecular studies of genes involved in CYN, GAA, MCs and ATX biosynthesis. Extracts of C. raciborskii LBY-Cr and A. gracile LBN-Ag caused a significant increase in the intracellular reactive oxygen content in human neutrophils during short-term (1 h) exposure and also led to lipid peroxidation and cell death. No cytotoxic effects were noted for the other tested strains. None of the toxin genes ( cyrA , cyrJ , anaF and mcyE ) and toxins (CYN, GAA, MCs, BMAA, ATX and STX) were detected. The only exception was DAB found at a concentration below 1.0 μg g − 1 dw in A. gracile LWI-Ag. It is the first time that cyanobacterial DAB producer has been identified in the Central European region. The study points to the production of as yet unknown metabolite(s) that may pose a relevant threat to human health through strains of C. raciborskii and A. gracile isolated from two Polish lakes, and adds to the general understanding of the toxicity of European strains of both species.

Published

2017

202. Non-enzymatic glutathione reactivity and in vitro toxicity: A non-animal approach to skin sensitization

Author

Aptula, Aynur O., Patlewicz, Grace, Roberts, David W., and Schultz, T.W.

Subjects

*TRANSFER factor (Immunology), *CONTACT dermatitis, *DELAYED hypersensitivity, *SKIN inflammation, *IMMUNOLOGY

Abstract

Abstract: The development of non-animal methods to predict the potential of chemicals to cause skin sensitization is of great importance. On the basis of many published studies into the underlying chemical mechanisms skin sensitization, the immunological priming which leads to the disease allergic contact dermatitis, is recognized as a reactive chemistry endpoint. Consequently, the combination of chemical assays with in vitro techniques may provide a useful surrogate to animal testing for skin sensitization. This study attempts to investigate the relationship between skin sensitization assessed in the local lymph node assay (LLNA) initially and a thiol reactivity index based on glutathione (GSH), pEC50 thiol (EC50 being defined as the concentration of the test substance which gives 50% depletion of free thiol under standard conditions) in combination with a measure of cytotoxicity (pIGC50) to Tetrahymena pyriformis (TETRATOX). The pEC50 thiol values and the pIGC50 values were determined for twenty-four compounds for which LLNA test data were available. Thiol reactivity was found to discriminate sensitizers from non-sensitizers according to the rule: pEC50 thiol>−0.55 indicates that the compound will be a skin sensitizer. However, because of metabolic activation a pEC50 thiol<−0.55 does not necessarily mean that the compound will be a non-sensitizer. Excess toxicity to T. pyriformis (i.e. the extent of toxic potency over that expected by non-polar narcosis) was determined in order to assess biological reactivity. The best discrimination based on excess toxicity in the TETRATOX assay was given by the “rule”: excess toxicity>0.50 indicates that the compound will be a skin sensitizer. These approaches become more powerful when combined. When taken together, the thiol and TETRATOX assays predict the sensitization potential of 23 of the 24 compounds correctly. α-Hexylcinnamic aldehyde is incorrectly predicted to be a non-sensitizer, whereas LLNA results suggest it may be a weak sensitizer, this inaccuracy being rationalized in terms of its high hydrophobicity. Due to the selectivity of electro(nucleo)philic reactions some sensitizing compounds will not be identified using a single nucleophile such as thiol. [Copyright &y& Elsevier]

Published

2006

203. Microcystin-LR induced cellular effects in mammalian and fish primary hepatocyte cultures and cell lines: A comparative study

Author

Boaru, Daniela Alina, Dragoş, Nicolae, and Schirmer, Kristin

Subjects

*RAINBOW trout, *CELL lines, *MESSENGER RNA, *BACTERIAL toxins

Abstract

Abstract: The impact of microcystin-LR, one of the most common cyanobacterial toxins, on liver and gut cells originating from mammals and fish was compared. Upon exposure of human and rainbow trout (Oncorhynchus mykiss) cell lines up to 2.5μM microcystin-LR, no alteration in cell viability was observed as assessed with three fluorescent indicators dyes, CFDA-AM, Alamar Blue and neutral red. The lack of sensitivity of the trout cell lines coincided with an absence of detectable mRNA levels of organic anion transporter polypeptide (OATP), which is implicated in the uptake of microcystin-LR. In contrast to the cell lines, primary rainbow trout and mouse hepatocytes showed damage to subcellular structures, particularly the lysosomes, as indicated by neutral red. This led us to propose a thus far undetected role of lysosomes as targets and mediators of microcystin-LR elicited cellular damage. An inhibitor of OATP, rifampicin, partly protected hepatocytes from this damage. Yet, the sensitivity of rainbow trout hepatocytes rapidly declined in culture, accompanied by decreasing levels of OATP mRNA. The sensitivity of mouse hepatocytes toward microcystin-LR also declined in culture but overall was about 25-fold greater than that of the trout cells. These differences mirror those observed in vivo and suggest the use hepatocytes for deciphering the species differences. [Copyright &y& Elsevier]

Published

2006

204. In vitro toxicity of nanoparticles in BRL 3A rat liver cells

Author

Hussain, S.M., Hess, K.L., Gearhart, J.M., Geiss, K.T., and Schlager, J.J.

Subjects

*METALLIC oxides, *NANOPARTICLES, *MANGANESE oxides, *TUNGSTEN, *CELL morphology, *LACTATE dehydrogenase, *GLUTATHIONE

Abstract

Abstract: This study was undertaken to address the current deficient knowledge of cellular response to nanosized particle exposure. The study evaluated the acute toxic effects of metal/metal oxide nanoparticles proposed for future use in industrial production methods using the in vitro rat liver derived cell line (BRL 3A). Different sizes of nanoparticles such as silver (Ag; 15, 100nm), molybdenum (MoO3; 30, 150nm), aluminum (Al; 30, 103nm), iron oxide (Fe3O4; 30, 47nm), and titanium dioxide (TiO2; 40nm) were evaluated for their potential toxicity. We also assessed the toxicity of relatively larger particles of cadmium oxide (CdO; 1μm), manganese oxide (MnO2; 1–2μm), and tungsten (W; 27μm), to compare the cellular toxic responses with respect to the different sizes of nanoparticles with different core chemical compositions. For toxicity evaluations, cellular morphology, mitochondrial function (MTT assay), membrane leakage of lactate dehydrogenase (LDH assay), reduced glutathione (GSH) levels, reactive oxygen species (ROS), and mitochondrial membrane potential (MMP) were assessed under control and exposed conditions (24h of exposure). Results showed that mitochondrial function decreased significantly in cells exposed to Ag nanoparticles at 5–50μg/ml. However, Fe3O4, Al, MoO3 and TiO2 had no measurable effect at lower doses (10–50μg/ml), while there was a significant effect at higher levels (100–250μg/ml). LDH leakage significantly increased in cells exposed to Ag nanoparticles (10–50μg/ml), while the other nanoparticles tested displayed LDH leakage only at higher doses (100–250μg/ml). In summary the Ag was highly toxic whereas, MoO3 moderately toxic and Fe3O4, Al, MnO2 and W displayed less or no toxicity at the doses tested. The microscopic studies demonstrated that nanoparticle-exposed cells at higher doses became abnormal in size, displaying cellular shrinkage, and an acquisition of an irregular shape. Due to toxicity of silver, further study conducted with reference to its oxidative stress. The results exhibited significant depletion of GSH level, reduced mitochondrial membrane potential and increase in ROS levels, which suggested that cytotoxicity of Ag (15, 100nm) in liver cells is likely to be mediated through oxidative stress. [Copyright &y& Elsevier]

Published

2005

205. Predicting the risk of developmental toxicity from in vitro assays

Author

Spielmann, Horst

Subjects

*RISK assessment, *TOXICITY testing, *REPRODUCTION, *DWARFISM

Abstract

Abstract: Reproductive toxicity refers to the adverse effects of a substance on any aspect of the reproductive cycle, including the impairment of reproductive function, the induction of adverse effects in the embryo, such as growth retardation, malformations, and death. Due to the complexity of the mammalian reproductive cycle, it is impossible to model the whole cycle in a single in vitro system in order to detect chemical effects on mammalian reproduction. However, the cycle can be broken down in its biological components which may be studied individually or in combination. This approach has the advantage that the target tissue/organ of a developmental toxicant can be identified. In specific areas of developmental toxicity, a number of useful and promising in vitro models are already available. The individual tests may be used as building blocks of a tiered testing strategy. So far, research has focused on developing and validating tests covering only a few components of the reproductive cycle, in particular organogenesis of the embryo, reflecting important concerns for teratogenic chemicals. During the last three decades, a number of established models and promising new developments have emerged that will be discussed, e.g. culture of mammalian embryos and embryonic cells and tissues and the use of embryonic stem cells. [Copyright &y& Elsevier]

Published

2005

206. In vitro cytotoxicity testing of airborne formaldehyde collected in serum-free culture media.

Author

Bakand, S., Hayes, A., Winder, C., Khalil, C., and Markovic, B.

Subjects

*FORMALDEHYDE, *CELL death, *FIBROBLASTS, *DISINFECTION & disinfectants, *CONNECTIVE tissue cells, *CELL culture, *TOXICITY testing

Abstract

The purpose of this study was to identify a suitable sampling model for on-site toxicity assessment of soluble air contaminants such as formaldehyde, a well known industrial and indoor air contaminant. The in vitro cytotoxicity of formaldehyde, the selected model for soluble air contaminants, was studied using the MTS (tetrazolium salt) assay in two carcinoma cell lines, A549 epithelial lung and HepG2 hepatocarcinoma, and in skin fibroblasts. The cytotoxic effects of airborne formaldehyde were evaluated using test atmospheres in concentrations below 10 ppm (12.3 mg/m3), generated by a dynamic diffusion method and bubbled (0.3 L/min) through serum-free culture media for one or four hours. Human cells were treated with formaldehyde air samples, and cell viability was determined after four hours incubation. In parallel, the concentration of airborne formaldehyde was monitored, using the 3500 NIOSH method. Cell viability of the HepG2 cells exposed to formaldehyde air samples (8.75 ppm × 4 h) was reduced to less than 50% (31.6±1.24%). The HepG2 cell lines were found to be more sensitive (IC50=103.79±23.55 mg/L) to formaldehyde than both A549 cell lines (IC50=198.36±9.54 mg/L) and skin fibroblasts (IC50=196.68±36.73 mg/L) (P<0.01). An average of 96.8% was determined for collection efficiency of formaldehyde in serum-free culture media. The results of this study suggest that absorption of soluble air contaminants, such as formaldehyde, in serum-free culture media can be used as a suitable sampling model for on-site toxicity assessments. [ABSTRACT FROM AUTHOR]

Published

2005

207. Effects of a desealant formulation, SR-51® and its individual components on the oxidative functions of mitochondria

Author

Moscova, M., Oakes, D.J., Pollak, J.K., and Webster, W.S.

Subjects

*SOLVENTS, *CHEMICALS, *MAINTENANCE, *ARMED Forces

Abstract

The Royal Australian Air Force has reported that personnel involved in F-111 fuel tank maintenance were concerned that exposure to a range of chemicals during the period 1977–mid-1990s was the cause of health problems. Particular concern was directed at a desealant chemical mixture known as SR-51®. The current study, using in vitro submitochondrial assays, was designed to investigate the relative toxicities of the four components of SR-51® (Aromatic 150 solvent (Aro150), dimethylacetamide (DMA), thiophenol (TP) and triethylphosphate (TEP)). Based on the EC50 values, TP and Aro150 were the most toxic components and were markedly more toxic than TEP and DMA. [Copyright &y& Elsevier]

Published

2004

208. Sperm bioassay for rapid detection of cereulide-producing Bacillus cereus in food and related environments

Author

Andersson, Maria A., Jääskeläinen, Elina L., Shaheen, Ranad, Pirhonen, Tuula, Wijnands, Luc M., and Salkinoja-Salonen, Mirja S.

Subjects

*BACILLUS cereus, *BIOLOGICAL assay, *ARTIFICIAL insemination, *SPERMATOZOA, *BACILLUS (Bacteria), *BOARS

Abstract

A novel in vitro method, sperm micro assay for rapidly distinguishing cereulide, the emetic toxin producing Bacillus cereus from non-producers is described and its use for quantitating cereulide and screening large numbers of B. cereus strains/colonies evaluated. The assay is non-laborious and can be executed with equipment present in most laboratories. Boar spermatozoa, purchased as standard semen from artificial insemination suppliers, are used to detect toxicity. Boar sperms respond within 5 min by cessation of motility when exposed at 37 °C to heat-treated (100 °C) extract prepared from a cereulide containing B. cereus. The assay can be done on individual colonies on the primary plate, with no need for pure culture and the qualitative result is obtained within 30 min. The assay is robust, not sensitive to age or storage of the culture plates. The use of the sperm micro assay for semiquantitative estimation of cereulide in B. cereus was validated with 14 different B. cereus strains using as reference the specific chemical assay for cereulide, based on liquid chromatography-ion trap mass spectrometry (LC-ion trap MS). The cereulide contents calculated from endpoint dilutions of the sperm micro assay matched the result of the chemical analysis closely. The detection threshold of the sperm micro assay was measured as 0.3±0.1 ng of cereulide per 5.4×106 sperm cells in 0.2 ml or 0.9 ng of cereulide per mg of B. cereus biomass (wet wt.). Food-related B. cereus strains contained 4–400 ng of cereulide per mg (wet wt.). When a large number of B. cereus of food, non-food, clinical and environmental origins were screened and 107 independent strains/isolates were identified as cereulide producers, it was observed that all of these had low or no haemolytic activity when cultivated on bovine blood agar. None of the strains/isolates with wide, clear zones of haemolysis, considered typical of B. cereus, produced cereulide. [Copyright &y& Elsevier]

Published

2004

209. Toxicity of a Treatment Associating Dopamine and Disulfiram for Catecholaminergic Neuroblastoma SH-SY5Y Cells: Relationships with 3,4-Dihydroxyphenylacetaldehyde Formation

Author

Legros, Hélène, Dingeval, Marie-George, Janin, François, Costentin, Jean, and Bonnet, Jean-Jacques

Subjects

*DOPAMINE, *DISULFIRAM, *NEUROBLASTOMA, *DRUG side effects, *THERAPEUTICS

Abstract

3,4-Dihydroxyphenylacetaldehyde (DOPAL) is formed by the oxidative deamination of dopamine (DA) catalyzed by monoamine oxidases (MAO); then, the aldehyde is oxidized to 3,4-dihydroxyphenylacetic acid (DOPAC) by aldehyde dehydrogenases (ALDH) or reduced to 3,4-dihydroxyphenylethanol (DOPET) by aldose/aldehyde reductases. The present work aimed at evaluating the in vitro toxicity of DOPAL on catecholaminergic neuroblastoma SH-SY5Y cells which accumulate DA. DOPAL synthesis was stimulated by incubating cells with DA and blocking DOPAL oxidation by disulfiram, an irreversible inhibitor of ALDH. As evidenced by MTT reduction assays, DA and disulfiram treatments produced cell losses which increased with time. 10–2 M DA reduced by 40% cell viability after a 1 h treatment, when its TC50 (concentration reducing viability by 50%) value was 7.3×10−5 M after a 24 h treatment. For the same treatment periods, TC50 values for disulfiram were 8×10−5 and 8.7×10−7 M, respectively. MTT reduction assay performed after a 24 h treatment followed by a 24 h incubation in a drug-free medium evidenced that the toxicity of 10−4 M DA or 10−6 M disulfiram was potentiated by the second drug. HPLC measurements showed that DOPAL was produced at the early stages of the treatment by DA and disulfiram. This was evidenced by the significant increase in the (DOPAL+DOPET)/DOPAC ratio observed after a combined 3 h treatment by 10−4 M DA and 10−6 M disulfiram. Total contents in DA and DOPAL were greatly reduced at the end of a 15 h treatment, and disulfiram did not significantly enhanced the (DOPAL+DOPET)/DOPAC ratio. For both treatment durations, DOPAL and DOPET were detectable only in the extracellular medium. So, these results suggest that an early production of DOPAL could produce delayed toxic effects on SH-SY5Y cells. Production of DOPET and release of DOPAL could be important means for reducing DOPAL concentrations in dopaminergic neurons. [Copyright &y& Elsevier]

Published

2004

210. A comparison of in vitro toxicities of cigarette smoke condensate from Eclipse cigarettes and four commercially available ultra low-“tar” cigarettes

Author

Foy, J.W.D., Bombick, B.R., Bombick, D.W., Doolittle, D.J., Mosberg, A.T., and Swauger, J.E.

Subjects

*TOXICITY testing, *CIGARETTES, *CIGARETTE smokers, *TOBACCO, *TOXICOLOGY

Abstract

Eclipse is a cigarette that primarily heats rather than burns tobacco. R.J. Reynolds Tobacco Company (RJRT) has previously reported the results of in vitro toxicity studies comparing Eclipse with University of Kentucky 1R5F and 1R4F reference cigarettes. To characterize the differences between Eclipse and very low yielding/ultra low-“tar” (vULT) tobacco-burning cigarettes, RJRT conducted a comparative evaluation of the genotoxicity and cytotoxicity of mainstream cigarette smoke condensate (CSC) from Eclipse and three vULT tobacco-burning cigarettes (Now 83 Box, Merit Ultima and Carlton Soft Pack) as well as the leading ultra low-“tar” (ULT) brandstyle (Marlboro Ultra Lights) under four smoking regimens: (1) FTC—35 ml puff volume every 60 s for a 2 s duration (35/60/2); (2) 50/30/2, 0% vents blocked; (3) Massachusetts—45/30/2, 50% vents blocked; (4) Canadian—55/30/2, 100% vents blocked. Ames testing indicated that Eclipse CSC was less (P<0.05) mutagenic than CSC from the four cigarettes under all smoking regimens when compared on a revertants per mg Total Particulate Matter (TPM) basis. When mutagenicity was calculated on a revertants per cigarette basis the mutagenicity of Eclipse CSC was lower (P<0.05) than the mutagenicity of Merit Ultima, Carlton Soft Pack, and Marlboro Ultra Lights, regardless of the puffing regimen. On a per cigarette basis, the calculated mutagenicity of Eclipse was higher (P<0.05) than Now 83 Box cigarettes in the FTC and 50/30/2 regimens but lower (P<0.05) in the Massachusetts and Canadian regimens. Eclipse CSC was less (P<0.05) cytotoxic as measured in the neutral red assay (based on EC50 values—μg TPM/ml media) than the CSC from the four test cigarettes regardless of the regimen used. Collectively, these data demonstrate that the toxicity of CSC from Eclipse is significantly reduced relative to the activity of CSC from the tested vULT cigarettes and the Marlboro Ultra Lights. [Copyright &y& Elsevier]

Published

2004

211. N-Fatty Acylation of Hydrolyzed Fumonisin B1, But Not of Intact Fumonisin B1, Strongly Enhances In Vitro Mammalian Toxicity.

Author

Abou-Karam, Mohamed, Abbas, Hamed K., and Shier, W. Thomas

Subjects

*FUMONISINS, *MYCOTOXINS, *FUSARIUM, *TOXICOLOGY, *ACYLATION, *CERAMIDES

Abstract

Fumonisin B1 (FB1) is the most abundant of a series of sphingosine-analog mycotoxins produced by Fusarium verticillioides, the major fungal contaminant of stored corn (maize) world-wide. Fumonisins were originally isolated as environmental tumor promoters, and they remain a concern because they are frequent contaminants of corn-derived food products intended for direct human consumption. FB1 inhibits ceramide synthase, which may account for its acute toxic effects, but understanding of its tumor promotion mechanism has been limited by the general lack of understanding in the field. There is no evidence for functional metabolism of fumonisins in mammals, but abiogenic conversions during food processing are a concern because some known conversion products retain biological activity, including hydrolyzed FB1 (HFB1). HFB1, formed by alkaline removal of FB1 side chains, is a frequent contaminant of lime-treated corn products such as tortillas and tortilla chips. Humpf et al. (J. Biol. Chem., 273, 19060, 1998) observed that HFB1 not only inhibits ceramide synthase, but it is converted to a ceramide analog with about ten times the in vitro mammalian toxicity of intact FB1. In the present study we have confirmed this observation by preparing a series of ceramide analogs of HFB1 with varying fatty acid chain lengths and degree of unsaturation. Optimal in vitro mammalian toxicity was observed with fatty acid chain lengths of 10–14 carbons. However, ceramide analogs of HFB1 were not phytotoxic in vitro, and ceramide analogs of FB1 were not toxic in either mammalian or plant in vitro bioassays. [ABSTRACT FROM AUTHOR]

Published

2004

212. Effect of different toxic compounds on ATP content and acid phosphatase activity in axenic cultures of Tetrahymena pyriformis.

Author

Nicolau, Ana, Mota, Manuel, and Lima, Nelson

Subjects

PROTOZOA, ADENOSINE triphosphate, TOXICOLOGY, TETRAHYMENA

Abstract

The sensitivity of protozoa, and particularly ciliated protozoa, to environmental changes suggested a study on the physiological responses arising from exposure to toxic compounds. Tetrahymena pyriformis was used as a test organism in a set of miniaturized assays. The physiological response of this ciliate was assessed in terms of adenosine-5′-triphosphate content and acid phosphatase activity after exposure of the cultures of T. pyriformis to four toxicants: copper, zinc, Triton X-100, and cycloheximide. In the range of concentrations used, stimulation and inhibition of these two parameters were observed. The correlation between the two parameters is analyzed. [Copyright &y& Elsevier]

Published

2004

213. Evaluation of liver toxicity in vitro

Author

Kafuňková, Kateřina, Maixnerová, Jana, and Bárta, Pavel

Subjects

cytotoxicity, inhibition of metabolism, in vitro toxicity, in vitro toxicita, buněčné linie, cytotoxicita, inhibice metabolismu, cell lines

Abstract

Charles University Faculty of Pharmacy in Hradec Králové Department of Pharmacology and Toxicology Student: Kateřina Kafuňková Supervisor: RNDr. Jana Maixnerová, Ph.D. Title of diploma thesis: Evaluation of liver toxicity in vitro The subject of the diploma thesis is toxicity evaluation of newly synthesised substances on a cellular model representing a hepatocyte. The tested substances have been provided by the Department of Organic and Bioorganic Chemistry at the Faculty of Pharmacy in Hradec Králové, Charles University, as potential antifungal pharmaceuticals and medicine effective against Methicillin-resistant Staphylococcus aureus (MK-NO2-1, MK-NO2-2, DAB-5-K, PABA-Me-5, PABA-Et-5, MK-F-1, PABAN- 3, PABAN-5, MK-F-2, MK-CF3-1, MK-CF3- 2). In order to determine the toxicity we have implemented two methods. The first method is based upon measuring metabolic activity of cells by means of reducing tetrazolium to a colored product. The second method detects the amount of LDH released as a marker of toxicity. The human hepatoma cell line HepG2was used as a model. . The IC50 and EC50 parameters were used to assess the degree of viability and cytotoxicity. The final values obtained from the first method indicated all tested substances showed a certain level of toxicity to the hepatic tissue. MK-CF3-2 is the most...

Published

2020

214. Involvement of apoptosis in hydrazine induced toxicity in rat primary hepatocytes

Author

Hussain, Saber M. and Frazier, John M.

Subjects

*APOPTOSIS, *DNA, *CELL death, *CELL membranes, *IMMUNOSUPPRESSIVE agents

Abstract

The current study was undertaken to investigate the role of apoptosis in hydrazine induced hepatotoxicity. Hepatocytes were exposed to hydrazinium nitrate (HzN) at two doses (50 and 75 mM) for 2 h then placed in fresh HzN-free media and cultured for an additional 24 h. Post-exposure, cell viability was evaluated at several time points by lactate dehydrogenase (LDH) leakage and 3-(4,5-dimethylthiazol-2-yl)-2,5-diphenyltetrazolium bromide (MTT) reduction. Markers of apoptosis (mitochondrial membrane potential, annexin binding, DNA fragmentation, caspase activation, and cytochrome c release) were measured 24 h post-exposure. The viability data showed time dependent increase in LDH leakage at 75 mM of HzN, with only a slight increase at 50 mM. MTT reduction showed a decrease in mitochondrial activity at both doses immediately after the 2 h continous exposure. However, MTT reduction returned to normal at 50 mM while at 75 mM, MTT reduction initially recovered but then deteriorated to approximately 50% of controls at 24 h post-exposure. Based on viability data, exposure to 50 mM HzN for 2 h is a marginally toxic dose while 75 mM is a significantly toxic dose. The results for apoptosis biomarkers showed a reduction in mitochondrial membrane potential, an increase in annexin binding, an increase in total caspase activity, moderate activation of caspase-3, and release of cytochrome c. However, the appearance of DNA fragmentation in HzN exposed cells was very low compared to positive controls (cadmium and cyclosporine). The possibility that HzN induces apoptosis without the involvement of DNA fragmentation can not be ruled out. The present results, overall, suggest that apoptosis may be a contributing factor in acute HzN toxicity. [Copyright &y& Elsevier]

Published

2003

215. A New Hepatoma Cell Line for Toxicity Testing at Repeated Doses.

Author

Fabre, N., Arrivet, E., Trancard, J., Bichet, N., Roome, N.O., Prenez, A., and Vericat, J.-A.

Published

2003

216. Risk Assessment of High-Energy Chemicals by in Vitro Toxicity Screening and Quantitative Structure-Activity Relationships.

Author

Trohalaki, Steven, Zellmer, Robert J., Pachter, Ruth, Hussain, Saber M., and Frazier, John M.

Subjects

HYDRAZINE, CHEMICALS, QSAR models, MITOCHONDRIA, REACTIVE oxygen species

Abstract

Hydrazine propellants pose a substantial operational concern to the U.S. Air Force and to the aerospace industry because of their toxicity. In our continuing efforts to develop methods for the prediction of the toxicological response to such materials, we have measured in vitro toxicity endpoints for a series of high-energy chemicals (HECs) that were recently proposed as propellants. The HECs considered are structurally diverse and can be classified into four chemical types (hydrazine-based, amino-based, triazoles, and a quaternary ammonium salt), although most are hydrazine derivatives. We measured the following endpoints in primary cultures of isolated rat hepatocytes: mitochondrial function (MTT), lactate dehydrogenase leakage (LDH), generation of reactive oxygen species (ROS), and total glutathione content (GSH). In several instances, effective concentrations (EC) were indeterminate, and only lower limits to the measured endpoints could be ascertained. Using molecular descriptors calculated with a semiempirical molecular orbital method, quantitative structure-activity relationships (QSARs) were derived for MTT (EC25) and for GSH (EC50). Correlation coefficients for 2- and 3-parameter QSARs of about 0.9 enable us to predict the toxicity for similar compounds. Furthermore, except in one case, predicted EC values for the uncertain endpoints were consistent with experiment. Descriptors comprising the QSARs for MTT were consistent with the biophysical mechanism of toxic response found experimentally for hydrazine derivatives. Application of our derived QSARs will assist in predicting toxicity for newly proposed propellants. [ABSTRACT FROM PUBLISHER]

Published

2002

217. 3-Nitropropionic Acid Neurotoxicity in Hippocampal Slice Cultures: Developmental and Regional Vulnerability and Dependency on Glucose

Author

Noer, Helle, Kristensen, Bjarne W., Noraberg, Jens, Zimmer, Jens, and Gramsbergen, Jan Bert

Subjects

*NEUROTOXICOLOGY, *HIPPOCAMPUS (Brain)

Abstract

We investigated whether neurotoxic effects of the mitochondrial toxin 3-nitropropionic acid (3-NP) in hippocampal slice cultures are dependent on glucose levels in the culture medium and whether such effects occur via apoptosis or necrosis. In addition, 3-NP toxicity was investigated at two developmental stages of the cultures, prepared from rat brain at postnatal day 5–7 and grown in Neurobasal medium for 1 or 3 weeks. Cultures were exposed to 3-NP in the presence of high (25 mM), normal (5 mM), or low (3 mM) glucose for 48 h, followed by 48 h incubation in medium without 3-NP. Cellular propidium iodide (PI) uptake and lactate dehydrogenase (LDH) efflux into the medium revealed time- and dose-dependent cell death by 3-NP, with EC50 values of about 60 μM in high or normal glucose. Regional vulnerability, as assessed by PI uptake and MAP2 immunostaining, in 3-week-old cultures was as follows: CA1 > CA3 > fascia dentata. In low glucose much lower concentrations of 3-NP (25 μM) triggered neurotoxicity. One-week-old cultures were less susceptible to 3-NP toxicity than 3-week-old cultures, but the dentate granule cells were relatively more affected in the immature cultures. We found no evidence for apoptotic cell death by 3-NP in 3-week-old cultures, but in 1-week-old cultures the putative apoptotic marker c-JUN/AP1 and nuclear fragmentation (Hoechst) were significantly increased in the dentate granule cells. [Copyright &y& Elsevier]

Published

2002

218. Biological effects of cellulose nanofibrils in a lung epithelial cell line

Author

Teixeira, Sara Antunes Almeida, Silva, Maria João, and Louro, Maria Henriqueta

Subjects

nanotechnology, biological effects, cellulose nanofibrils, safety assessment, A549 cells, in vitro toxicity, Engenharia e Tecnologia::Engenharia Médica [Domínio/Área Científica]

Abstract

Cellulose nanofibrils (CNFs) are plant-derived nanomaterials, showing advantageous physicochemical properties, renewable nature and low cost. CNFs have great potential in several industries, including forest, food, pharmaceutical and biomedicine, as drug-delivery systems or for tissue repair and regeneration. The increased production and application of CNFs leads to greater exposure of both workers and consumers, being extremely important to evaluate possible negative outcomes for human health. Due to their similarities with other fibers, such as carbon nanotubes, they may reveal adverse effects, such as carcinogenesis. The objective of this work was to evaluate the biosafety of CNFs produced by different pre-treatments - TEMPO-mediated oxidation and enzymatic hydrolysis - from a bleached industrial Eucalyptus globulus kraft pulp. For this purpose, the internalization, cytotoxicity and genotoxicity of these CNFs was analysed through different parameters: intracellular localization, cell viability and chromosome damage. Human lung epithelial cells (A549) were used, since the most frequent route of exposure is inhalation of CNFs, especially in occupational context

Published

2019

219. Design, Synthesis and In Vitro Mechanistic Investigation of Novel Hexacyclic Cage-Like Hybrid Heterocycles

Author

Abdulrahman I. Almansour, Suresh Kumar Raju, Arumugam Natarajan, and Faruq Mohammad

Subjects

Thiosemicarbazones, Programmed cell death, apoptotic mechanism, Pharmaceutical Science, Antineoplastic Agents, in vitro toxicity, 01 natural sciences, Jurkat cells, Article, Analytical Chemistry, lcsh:QD241-441, 03 medical and health sciences, Jurkat Cells, lcsh:Organic chemistry, Neoplasms, Drug Discovery, Humans, Physical and Theoretical Chemistry, [3 + 2] cycloaddition, hexacyclic cage-like hybrid heterocycles, 030304 developmental biology, 0303 health sciences, Cycloaddition Reaction, Molecular Structure, 010405 organic chemistry, Cell growth, Chemistry, Acenaphthenes, role of caspases, Organic Chemistry, Biological activity, Combinatorial chemistry, In vitro, Cycloaddition, 0104 chemical sciences, anticancer activity, Chemistry (miscellaneous), Apoptosis, A549 Cells, Cancer cell, Molecular Medicine, Azo Compounds

Abstract

Novel hexacyclic cage-like hybrid heterocycles have been synthesized in excellent yields employing a relatively less explored non-stabilized azomethine ylides derived from acenaphthenequinone and tyrosine with functionalized dipolarophiles using [3 + 2] cycloaddition strategy. The synthesized hexacyclic cage-like hybrid heterocycles were characterized by spectroscopic analysis. Following the physical characterization, these cage-like hybrid heterocycles were tested for their biological activity by means of different cancer (A549 and Jurkat cells) and non-cancer (BRL-3A and PCS-130) in vitro cell culture systems. The results of the study under tested concentrations (up to 100 &mu, M) indicated that these compounds are not affecting any viability to the cell growth of non-cancer cells, while providing significant anticancer activity against both of the cancer cells. Further analysis of in-depth mechanistic study for the cell death indicated that these compounds are exhibiting late apoptosis or early necrosis pathway to the cells where it is operated by the induction of caspases.

Published

2019

220. Silica Nanoparticles Provoke Cell Death Independent of p53 and BAX in Human Colon Cancer Cells

Author

Silvia Diabaté, Zhen An, Ravindra Peravali, Marco Al-Rawi, Carsten Weiss, Jin Yan, Susanne Fritsch-Decker, and Iris Hansjosten

Subjects

Life sciences, biology, Programmed cell death, General Chemical Engineering, in vitro toxicity, 02 engineering and technology, colon cells, Article, lcsh:Chemistry, 03 medical and health sciences, In vivo, ddc:570, medicine, Cytotoxic T cell, General Materials Science, Cytotoxicity, Caspase, 030304 developmental biology, Cisplatin, 0303 health sciences, Chemistry, respiratory system, 021001 nanoscience & nanotechnology, In vitro, synthetic amorphous silica, cell death, lcsh:QD1-999, Apoptosis, biology.protein, Cancer research, nanoparticles, 0210 nano-technology, medicine.drug

Abstract

Several in vitro studies have suggested that silica nanoparticles (NPs) might induce adverse effects in gut cells. Here, we used the human colon cancer epithelial cell line HCT116 to study the potential cytotoxic effects of ingested silica NPs in the presence or absence of serum. Furthermore, we evaluated different physico-chemical parameters important for the assessment of nanoparticle safety, including primary particle size (12, 70, 200, and 500 nm) and surface modification (&ndash, NH2 and &ndash, COOH). Silica NPs triggered cytotoxicity, as evidenced by reduced metabolism and enhanced membrane leakage. Automated microscopy revealed that the silica NPs promoted apoptosis and necrosis proportional to the administered specific surface area dose. Cytotoxicity of silica NPs was suppressed by increasing amount of serum and surface modification. Furthermore, inhibition of caspases partially prevented silica NP-induced cytotoxicity. In order to investigate the role of specific cell death pathways in more detail, we used isogenic derivatives of HCT116 cells which lack the pro-apoptotic proteins p53 or BAX. In contrast to the anticancer drug cisplatin, silica NPs induced cell death independent of the p53&ndash, BAX axis. In conclusion, silica NPs initiated cell death in colon cancer cells dependent on the specific surface area and presence of serum. Further studies in vivo are warranted to address potential cytotoxic actions in the gut epithelium. The unintended toxicity of silica NPs as observed here could also be beneficial. As loss of p53 in colon cancer cells contributes to resistance against anticancer drugs, and thus to reoccurrence of colon cancer, targeted delivery of silica NPs could be envisioned to also deplete p53 deficient tumor cells.

Published

2019

221. Chemical composition and ecotoxicity of plastic and car tire rubber leachates to aquatic organisms

Author

Andy M. Booth, Kongalage Don Ranil Jayasena, Elena Fabbri, Marco Capolupo, Lisbet Sørensen, Capolupo M., Sorensen L., Jayasena K.D.R., Booth A.M., and Fabbri E.

Subjects

Microplastics, Aquatic Organisms, Environmental Engineering, 0208 environmental biotechnology, 02 engineering and technology, 010501 environmental sciences, Plastic, 01 natural sciences, chemistry.chemical_compound, Raphidocelis subcapitata, Microalgae, Animals, Waste Management and Disposal, Marine mussel, Ecosystem, 0105 earth and related environmental sciences, Water Science and Technology, Civil and Structural Engineering, biology, Animal, Aquatic Organism, Ecological Modeling, Aquatic ecosystem, Plasticizer, Mussel, biology.organism_classification, In vitro toxicity, Pollution, Mytilus, 020801 environmental engineering, Polyvinyl chloride, chemistry, Plastic additive, Automobile, Environmental chemistry, Rubber, Ecotoxicity, Automobiles, Plastics, Dissolution, Water Pollutants, Chemical

Abstract

Synthetic polymer-based materials are ubiquitous in aquatic environments, where weathering processes lead to their progressive fragmentation and the leaching of additive chemicals. The current study assessed the chemical content of freshwater and marine leachates produced from car tire rubber (CTR), polypropylene (PP), polyethylene terephthalate (PET), polystyrene (PS) and polyvinyl chloride (PVC) microplastics, and their adverse effects on the microalgae Raphidocelis subcapitata (freshwater) and Skeletonema costatum (marine) and the Mediterranean mussel Mytilus galloprovincialis. A combination of non-target and target chemical analysis revealed a number of organic and metal compounds in the leachates, including representing plasticizers, antioxidants, antimicrobials, lubricants, and vulcanizers. CTR and PVC materials and their corresponding leachates had the highest content of tentatively identified organic additives, while PET had the lowest. The metal content varied both between polymer leachates and between freshwater and seawater. Notable additives identified in high concentrations were benzothiazole (CTR), phthalide (PVC), acetophenone (PP), cobalt (CTR, PET), zinc (CTR, PVC), lead (PP) and antimony (PET). All leachates, except PET, inhibited algal growth with EC50 values ranging from 0.5% (CTR) and 64% (PP) of the total leachate concentration. Leachates also affected mussel endpoints, including the lysosomal membrane stability and early stages endpoints as gamete fertilization, embryonic development and larvae motility and survival. Embryonic development was the most sensitive parameter in mussels, with EC50 values ranging from 0.8% (CTR) to 65% (PET) of the total leachate. The lowest impacts were induced on D-shell larvae survival, reflecting their ability to down-regulate motility and filtration in the presence of chemical stressors. This study provides evidence of the relationship between chemical composition and toxicity of plastic/rubber leachates. Consistent with increasing contamination by organic and inorganic additives, the leachates ranged from slightly to highly toxic to mussels and algae, highlighting the need for a better understanding of the overall impact of plastic-associated chemicals on aquatic ecosystems.

Published

2019

222. In Vitro Toxicity of TiO2:SiO2 Nanocomposites with Different Photocatalytic Properties

Author

Bengalli, Ortelli, Blosi, Costa, Mantecca, Fiandra, Bengalli, R, Ortelli, S, Blosi, M, Costa, A, Mantecca, P, and Fiandra, L

Subjects

General Chemical Engineering, Nanoparticle, in vitro toxicity, 02 engineering and technology, Nanomaterials, lcsh:Chemistry, 03 medical and health sciences, chemistry.chemical_compound, Dynamic light scattering, General Materials Science, Viability assay, Cytotoxicity, 030304 developmental biology, 0303 health sciences, safe(r)-by-design, Nanocomposite, Chemistry, nanoparticle, technology, industry, and agriculture, 021001 nanoscience & nanotechnology, Chemical engineering, lcsh:QD1-999, Titanium dioxide, Photocatalysis, nanoparticles, 0210 nano-technology

Abstract

The enormous technological relevance of titanium dioxide (TiO2) nanoparticles (NPs) and the consequent concerns regarding potentially hazardous effects that exposure during production, use, and disposal can generate, encourage material scientists to develop and validate intrinsically safe design solution (safe-by-design). Under this perspective, the encapsulation in a silica dioxide (SiO2) matrix could be an effective strategy to improve TiO2 NPs safety, preserving photocatalytic and antibacterial properties. In this work, A549 cells were used to investigate the toxic effects of silica-encapsulated TiO2 having different ratios of TiO2 and SiO2 (1:1, 1:3, and 3:1). NPs were characterized by electron microscopy and dynamic light scattering, and cell viability, oxidative stress, morphological changes, and cell cycle alteration were evaluated. Resulting data demonstrated that NPs with lower content of SiO2 are able to induce cytotoxic effects, triggered by oxidative stress and resulting in cell necrosis and cell cycle alteration. The physicochemical properties of NPs are responsible for their toxicity. Particles with small size and high stability interact with pulmonary cells more effectively, and the different ratio among silica and titania plays a crucial role in the induced cytotoxicity. These results strengthen the need to take into account a safe(r)-by-design approach in the development of new nanomaterials for research and manufacturing.

Published

2019

223. In Vitro Toxicity of TiO

Author

Rossella, Bengalli, Simona, Ortelli, Magda, Blosi, Anna, Costa, Paride, Mantecca, and Luisa, Fiandra

Subjects

safe(r)-by-design, nanoparticles, in vitro toxicity, Article

Abstract

The enormous technological relevance of titanium dioxide (TiO2) nanoparticles (NPs) and the consequent concerns regarding potentially hazardous effects that exposure during production, use, and disposal can generate, encourage material scientists to develop and validate intrinsically safe design solution (safe-by-design). Under this perspective, the encapsulation in a silica dioxide (SiO2) matrix could be an effective strategy to improve TiO2 NPs safety, preserving photocatalytic and antibacterial properties. In this work, A549 cells were used to investigate the toxic effects of silica-encapsulated TiO2 having different ratios of TiO2 and SiO2 (1:1, 1:3, and 3:1). NPs were characterized by electron microscopy and dynamic light scattering, and cell viability, oxidative stress, morphological changes, and cell cycle alteration were evaluated. Resulting data demonstrated that NPs with lower content of SiO2 are able to induce cytotoxic effects, triggered by oxidative stress and resulting in cell necrosis and cell cycle alteration. The physicochemical properties of NPs are responsible for their toxicity. Particles with small size and high stability interact with pulmonary cells more effectively, and the different ratio among silica and titania plays a crucial role in the induced cytotoxicity. These results strengthen the need to take into account a safe(r)-by-design approach in the development of new nanomaterials for research and manufacturing.

Published

2019

224. In Vitro Toxicity Study of a Porous Iron(III) Metal‒Organic Framework

Author

Jian Ni, Xingbin Yin, Changhai Qu, Xin Leng, Xiaoxv Dong, Juyuan Luo, Longtai You, Gongsen Chen, and Hongliang Huang

Subjects

Models, Molecular, Biocompatibility, Cell Survival, Iron, Pharmaceutical Science, Apoptosis, in vitro toxicity, Article, Analytical Chemistry, Cell Line, lcsh:QD241-441, chemistry.chemical_compound, lcsh:Organic chemistry, Drug Discovery, Toxicity Tests, Humans, MTT assay, DAPI, Physical and Theoretical Chemistry, Particle Size, Cytotoxicity, Cell Shape, HepG2 cells, Metal-Organic Frameworks, HL-7702 cells, Chemistry, MIL-100(Fe), Organic Chemistry, Cell Membrane, In vitro, Staining, Chemistry (miscellaneous), Cell culture, Molecular Medicine, Drug carrier, Porosity, Nuclear chemistry

Abstract

A MIL series metal‒organic framework (MOF), MIL-100(Fe), was successfully synthesized at the nanoscale and fully characterized by TEM, TGA, XRD, FTIR, DLS, and BET. A toxicological assessment was performed using two different cell lines: human normal liver cells (HL-7702) and hepatocellular carcinoma (HepG2). In vitro cytotoxicity of MIL-100(Fe) was evaluated by the MTT assay, LDH releasing rate assay, DAPI staining, and annexin V/PI double staining assay. The safe dose of MIL-100(Fe) was 80 μg/mL. It exhibited good biocompatibility, low cytotoxicity, and high cell survival rate (HL-7702 cells’ viability &gt, 85.97%, HepG2 cells’ viability &gt, 91.20%). Therefore, MIL-100(Fe) has a potential application as a drug carrier.

Published

2019

225. Nicotine Exerts Cytotoxic Effects in a Panel of Healthy Cell Lines and Strong Irritating Potential on Blood Vessels.

Author

Chioran D, Sitaru A, Macasoi I, Pinzaru I, Sarau CA, Dehelean C, Dinu S, Szuhanek C, Zetu IN, Serafin AC, Rivis M, Poenaru M, and Dragoi R

Subjects

Animals, Cell Line, Chickens, Chorioallantoic Membrane, Female, Irritants, Antineoplastic Agents pharmacology, Nicotine toxicity

Abstract

The use of tobacco products is a major global public health issue, as it is the leading cause of preventable death worldwide. In addition, nicotine (NIC) is a key component of electronic and conventional cigarettes. Although nicotine's addictive potential is well known, its health effects are not entirely understood. Thus, the main objective of the present study was to evaluate its toxicological profile both in vitro, at the level of three healthy cell lines, and in ovo, at the level of the chorioallantoic membrane. Five different concentrations of nicotine were used in keratinocytes, cardiomyocytes, and hepatocytes for the purpose of evaluating cell viability, cell morphology, and its impact on nuclei. Additionally, the hen's egg test on the chorioallantoic membrane (HET-CAM) method was used to assess the biocompatibility and irritant potential of the chorioallantoic membrane. Across all cell lines studied, nicotine was proven to be significantly damaging to cell viability, with the highest concentration tested resulting in less than 2% viable cells. Moreover, the morphology of cells changed dramatically, with alterations in their shape and confluence. Nicotine-induced cell death appears to be apoptotic, based on its impact on the nucleus. In addition, nicotine was also found to have a very strong irritating effect on the chorioallantoic membrane. In conclusion, nicotine has an extremely strong toxicological profile, as demonstrated by the drastic reduction of cell viability and the induction of morphological changes and nuclear alterations associated with cellular apoptosis. Additionally, the HET-CAM method led to the observation of a strong irritating effect associated with nicotine.

Published

2022

226. Amphotericin B release rate is the link between drug status in the liposomal bilayer and toxicity.

Author

Svirkin Y, Lee J, Marx R, Yoon S, Landrau N, Kaisar MA, Qin B, Park JH, Alam K, Kozak D, Wang Y, Xu X, Zheng J, and Rivnay B

Abstract

Amphotericin B (AmB) is an amphiphilic drug commonly formulated in liposomes and administered intravenously to treat systemic fungal infections. Recent studies on the liposomal drug product have shed light on the AmB aggregation status in the bilayer, which heat treatment (curing) modifies. Although toxicity was found related to aggregation status - loose aggregates significantly more toxic than tight aggregates - the precise mechanism linking aggregation and toxicity was not well understood. This study directly measured drug release rate from various AmB liposomal preparations made with modified curing protocols to evaluate correlations among drug aggregation state, drug release, and in vitro toxicity. UV-Vis spectroscopy of these products detected unique curing-induced changes in the UV spectral features: a ∼25 nm blue-shift of the main absorption peak (λ max ) in aqueous buffer and a decrease in the OD 346 /OD 322 ratio upon thermal curing, reflecting tighter aggregation. In vitro release testing (IVRT) data showed, by applying and fitting first-order release kinetic models for one or two pools, that curing impacts two significant changes: a 3-5-fold drop in the overall drug release rate and a ten-fold decrease in the ratio between the loosely aggregated and the tightly aggregated, more thermodynamically stable drug pool. The kinetic data thus corroborated the trend independently deduced from the UV-Vis spectral data. The in vitro toxicity assay indicated a decreased toxicity with curing, as shown by the significantly increased concentration, causing half-maximal potassium release (TC 50 ). The data suggest that the release of AmB requires dissociation of the tight complexes within the bilayer and that the reduced toxicity relates to this slower rate of dissociation. This study demonstrates the relationship between AmB aggregation status within the lipid bilayer and drug release (directly measured rate constants), providing a mechanistic link between aggregation status and in vitro toxicity in the liposomal formulations., Competing Interests: The authors report no conflicts of interest. The authors alone are responsible for the content and writing of this article. This article reflects the authors' views and should not be construed to represent the FDA's views or policies., (© 2022 Shenyang Pharmaceutical University.)

Published

2022

227. In Vitro Nephrotoxicity and Permeation of Vancomycin Hydrochloride Loaded Liposomes.

Author

Papp N, Panicker J, Rubino J, Pais G, Czechowicz A, Prozialeck WC, Griffin B, Weissig V, Scheetz M, and Joshi MD

Abstract

Drugs can be toxic to the fetus depending on the amount that permeates across the maternal-fetal barrier. One way to limit the amount which penetrates this barrier is to increase the molecular size of the drug. In this study, we have achieved this by encapsulating our model antibiotic (vancomycin hydrochloride, a known nephrotoxic agent) in liposomes. PEGylated and non-PEGylated liposomes encapsulating vancomycin hydrochloride were prepared using two different methods: thin-film hydration followed by the freeze-thaw method and the reverse-phase evaporation method. These liposomes were characterized by their hydrodynamic size and zeta potential measurements, CryoTEM microscopy, loading and encapsulation efficiency studies, in vitro release measurements and in vitro cytotoxicity assays using NRK-52 E rat kidney cells. We also determined the in vitro permeability of these liposomes across the human placental cell and dog kidney cell barriers. Vancomycin hydrochloride-loaded PEGylated liposomes (VHCL-lipo) of a size less than 200 nm were prepared. The VHCL-lipo were found to have the faster release of vancomycin hydrochloride and resulted in greater viability of NRK-52E cells. In vitro, the VHCL-lipo permeated the human placental cell and dog kidney cell barriers to a lesser extent than the free vancomycin hydrochloride. The data suggest a reduction in nephrotoxicity and permeability of vancomycin hydrochloride after encapsulation in PEGylated liposomes.

Published

2022

228. Tiered testing of micro- and nanoplastics using intestinal in vitro models to support hazard assessments.

Author

Bredeck, Gerrit, Halamoda-Kenzaoui, Blanka, Bogni, Alessia, Lipsa, Dorelia, and Bremer-Hoffmann, Susanne

Subjects

*INTESTINES, *RISK assessment, *HIGH throughput screening (Drug development), *BIOLOGICAL systems, *CELL culture

Abstract

[Display omitted] • Intestinal in vitro toxicity studies mainly use Caco-2, HT29 or HCT116 monocultures. • Cytotoxicity, barrier permeability and transport mechanisms are the main endpoints. • Co-cultures, organ on a chip and organoids might increase the physiological relevance. • Effects involving the microbiome or specific cell types are difficult to assess. • Hazard identification of microplastics in vitro requires a tiered testing approach. The uncertainty of potential risks associated with micro- and nanoplastics (MNPs) are of growing public concern. However, the diversity of MNPs in the environment makes a systematic analysis of potential health effects challenging. New tools and approaches are necessary to investigate biological effects of MNPs. With this quick scoping review, we aim to analyse the suitability of in vitro models for assessing the interaction of MNPs with intestinal cells. Our analysis revealed that currently the majority of in vitro tests are based on the three cell lines Caco-2, HT-29, and HCT-116. They have particularly been used to assess endpoints related to basal cytotoxicity, the internalisation of MNPs and effects on the intestinal barrier. When co-cultured with various cell lines, they also allow to investigate additional effects such as inflammation, metabolic actions and the relevance of the intestinal mucus. However, methodological gaps remain regarding the assessment of a potential accumulation of MNPs, leaching of additives/impurities and in resulting long-term effects as well as cell-type specific toxicities. In addition, only few in vitro studies investigated effects of MNPs on the microbiome. Stem cell-based assays using, for example, the emerging organoid technology are promising for analysing MNP effects on tissue-like structures, while avoiding the particular characteristics of the currently used cancer derived cell lines. The various cell lines and culture techniques can be combined in testing strategies, to better elucidate potential biological interaction of MNPs with biological systems. We suggest to implement a tiered testing strategy, in which monocultures can serve as a tool for high-throughput testing of MNPs. In the next steps co-cultures can be used to assess the potential of a systemic uptake of MNPs and organ-on-a-chip models will provide more reliable insights into relevant doses triggering biological effects. Finally, organoids can help to discover new and more complex reactions initiated by MNPs. [ABSTRACT FROM AUTHOR]

Published

2022

229. A sensitive electrochemical sensor for environmental toxicity monitoring based on tungsten disulfide nanosheets/hydroxylated carbon nanotubes nanocomposite.

Author

Wu, Guanlan, Zheng, Huizi, Xing, Yi, Wang, Chengzhi, Yuan, Xing, and Zhu, Xiaolin

Subjects

*ELECTROCHEMICAL sensors, *CARBON nanotubes, *TUNGSTEN trioxide, *ENVIRONMENTAL monitoring, *NANOSTRUCTURED materials, *TUNGSTEN alloys, *MULTIWALLED carbon nanotubes, *TUNGSTEN

Abstract

There has been growing concern about the toxic effects of pollutants in the aquatic environment. In this study, a novel cell-based electrochemical sensor was developed to detect the toxicity of contaminants in water samples. A screen-printed carbon electrode, which was low-cost, energy-efficient, and disposable, was modified with tungsten disulfide nanosheets/hydroxylated multi-walled carbon nanotubes (WS 2 /MWCNTs-OH) to improve electrocatalytic performance and sensitivity. The surface morphology, structure, and electrochemical property of WS 2 /MWCNTs-OH composite film were characterized by emission scanning electron microscopy, transmission electron microscopy, energy dispersive spectroscopy, X-ray diffraction, Raman spectroscopy, and electrochemical impedance spectroscopy. Grass carp kidney cell line was utilized as the sensor biorecognition element to determine the electrochemical signals and evaluate cell viability. The sensor was used to detect the toxicity of one typical contaminant (2,4,6-trichlorophenol) and two emerging contaminants (bisphenol AF and polystyrene nanoplastics). The 48 h half inhibitory concentration (IC 50) values were 169.96 μM, 21.88 μM, and 123.01 μg mL−1, respectively, which were lower than those of conventional MTT assay, indicating the higher sensitivity of the proposed sensor. Furthermore, the practical application of the sensor was evaluated in chemical wastewater samples. This study provides an up-and-coming tool for environmental toxicity monitoring. [Display omitted] • A sensor based on tungsten disulfide nanosheets/carbon nanotubes was developed. • The electrochemical response mechanism of CIK cells was elucidated. • The cytotoxicity of 2,4,6-TCP, BPAF, and PSNPs was evaluated by the sensor. • The sensor exhibited higher sensitivity than traditional MTT assay. • The sensor was successfully used to detect toxicity of actual wastewater samples. [ABSTRACT FROM AUTHOR]

Published

2022

230. An eco-friendly production of ZnO NRs using Knema andamanica (Warb) extracts for photocatalytic and anticancer applications.

Author

Govindaraj Sudha, Kattakgoundar, Ali, Saheb, Karunakaran, Gopalu, Kowsalya, Mariyappan, Kolesnikov, Evgeny, Gorshenkov, Mikhail V., Velmurugan, Thangavel, and Prasanna Rajeshkumar, Mohan

Subjects

*ZINC oxide, *ZINC ions, *CANCER cells, *ABSORPTION spectra, *NANOMEDICINE, *BACTERIAL cells, *CELL growth

Abstract

[Display omitted] • Biosynthesis of ZnO NRs using Knema andamanica (Warb) leaf extracts. • Obtained ZnO nanorods was found to be non-toxic. • Photocatalytic, antioxidant, and cytotoxicity were characterized. • ZnO NRs found to be an excellent photocatalytic, and anticancer nanomedicine. Lung cancer is one of the most serious medical problems, and it is caused primarily by uncontrolled cell growth. Every year, the death rate due to cancer is increasing regularly. Despite the fact that various cancer treatments are being developed. An effective chemotherapic treatment using nanoparticles for a potential cancer application is still in progress. The primary goal of this study was to synthesize ZnO NRs using plant aqueous leaf extracts, which induce its magnificent applications in biomedical and cancer treatment applications. The ZnO NRs are obtained by substituting the chemical substances for the conversion of zinc ions into ZnO NRs during obtaining them with the help of Knema andamanica (Warb) leaf extracts. The obtained ZnO NRs are confirmed by particle characterization methods such as XRD analysis, which concluded that the obtained ZnO NRs are pure, with increased particle crystalline nature. The FTIR analysis reveals strong absorption spectra in the range of 400–4000 cm−1. The TEM picture reveals the development of rod-like shaped ZnO NRs with a particle size of 20–200 nm. The in vitro toxicity assessment using zebrafish embryos showed very less death rate of 6.4% which confirms the non-toxic behavior of the ZnO NRs. Hence, the anticancer property of ZnO NRs was performed by using the A549 lung cancer cell line. The MTT, XTT, NRU, and LDH studies provide a wide range of understanding about the cell death cycle. Genotoxicity results concluded that procured ZnO NRs stimulated ROS and apoptosis towards cancer cells through various intrinsic gene developments. Antibacterial properties of ZnO NRs against various pathogens were analyzed and differentiated and the results concluded that the procured ZnO NRs reveal efficient bacterial cell growth inhibition. The antioxidant and photocatalytic property of ZnO NRs reveals promising free radical scavenging and increased catalytic activity. The green mediated synthesized ZnO NRs might offer promising implementations in medicinal areas. [ABSTRACT FROM AUTHOR]

Published

2021

231. In vitro toxicity of fibrous glaucophane

Author

Martin Harper, Alessandro F. Gualtieri, Monia Benassi, Serena Mirata, Monica Filaferro, Giovanni Vitale, Dario Di Giuseppe, Sonia Scarfì, Mark Bailey, Rossella Avallone, and Alessandro Zoboli

Subjects

Amphibole asbestos, Fibrous glaucophane, FPTI, Human lung cells, In vitro toxicity, 0301 basic medicine, Blueschist, Time Factors, Cell Survival, Glaucophane, Population, engineering.material, Toxicology, medicine.disease_cause, Asbestos, Cell Line, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Lactate dehydrogenase, medicine, Humans, education, Lung, Minerals, education.field_of_study, Dose-Response Relationship, Drug, Asbestos, Amphibole, Macrophages, Asbestos, Crocidolite, Epithelial Cells, Molecular biology, Oxidative Stress, 030104 developmental biology, chemistry, Cell culture, Toxicity, engineering, Pleura, 030217 neurology & neurosurgery, Oxidative stress

Abstract

The health hazard represented by the exposure to asbestos may also concern other minerals with asbestos-like crystal habit. One of these potentially hazardous minerals is fibrous glaucophane. Fibrous glaucophane is a major component of blueschist rocks of California (USA) currently mined for construction purposes. Dust generated by the excavation activities might potentially expose workers and the general public. The aim of this study was to determine whether fibrous glaucophane induces in vitro toxicity effects on lung cells by assessing the biological responses of cultured human pleural mesothelial cells (Met-5A) and THP-1 derived macrophages exposed for 24 h and 48 h to glaucophane fibres. Crocidolite asbestos was tested for comparison. The experimental configuration of the in vitro tests included a cell culture without fibres (i.e., control), cell cultures treated with 50 μg/mL (i.e., 15.6 μg/cm2) of crocidolite fibres and 25-50−100 μg/mL (i.e., 7.8−15.6–31.2 μg/cm2) of glaucophane fibres. Results showed that fibrous glaucophane may induce a decrease in cell viability and an increase in extra-cellular lactate dehydrogenase release in the tested cell cultures in a concentration dependent mode. Moreover, it was found that fibrous glaucophane has a potency to cause oxidative stress. The biological reactivity of fibrous glaucophane confirms that it is a toxic agent and, although it apparently induces lower toxic effects compared to crocidolite, exposure to this fibre may be responsible for the development of lung diseases in exposed unprotected workers and population.

Published

2021

232. A High-Throughput Toxicity Screen of 42 Per- and Polyfluoroalkyl Substances (PFAS) and Functional Assessment of Migration and Gene Expression in Human Placental Trophoblast Cells.

Author

Blake BE, Rickard BP, and Fenton SE

Abstract

Per- and polyfluoroalkyl substances (PFAS) have become ubiquitous environmental contaminants that have been associated with adverse pregnancy outcomes in women and experimental research models. Adverse developmental and reproductive outcomes have been investigated for relatively few PFAS, and such studies are not scalable to address the thousands of unique chemical structures. As the placenta has been reported as a PFAS target tissue, the human placental trophoblast JEG-3 cell line was employed in a high-throughput toxicity screen (HTTS) to evaluate the effects of 42 unique PFAS on viability, proliferation, and mitochondrial membrane potential (MMP). HTTS concentration-response curve fitting determined EC50 values for 79% of tested compounds for at least one of the three endpoints. Trophoblast migratory potential was evaluated for a subset of six prioritized PFAS using a scratch wound assay. Migration, measured as the percent of wound closure after 72 h, was most severely inhibited by exposure to 100 µM perfluorooctanoic acid (PFOA; 72% closure), perfluorooctanesulfonic acid (PFOS; 57% closure), or ammonium perfluoro-2-methyl-3-oxahexanoate (GenX; 79% closure). PFOA and GenX were subsequently evaluated for disrupted expression of 46 genes reported to be vital to trophoblast health. Disrupted regulation of oxidative stress was suggested by altered expression of GPEX1 (300 µM GenX and 3 µM GenX), GPER1 (300 µM GenX), and SOD1 and altered cellular response to xenobiotic stress was indicated by upregulation of the placental efflux transporter, ABCG2 (300 µM GenX, 3 µM GenX, and 100 µM PFOA). These findings suggest the placenta is potentially a direct target of PFAS exposure and indicate that trophoblast cell gene expression and function are disrupted at PFAS levels well below the calculated cytotoxicity threshold (EC50). Future work is needed to determine the mechanism(s) of action of PFAS towards placental trophoblasts., Competing Interests: The authors declare that the research was conducted in the absence of any commercial or financial relationships that could be construed as a potential conflict of interest., (Copyright © 2022 Blake, Rickard and Fenton.)

Published

2022

233. Unveiling the Toxicity of Fine and Nano-Sized Airborne Particles Generated from Industrial Thermal Spraying Processes in Human Alveolar Epithelial Cells.

Author

Bessa MJ, Brandão F, Fokkens PHB, Leseman DLAC, Boere AJF, Cassee FR, Salmatonidis A, Viana M, Monfort E, Fraga S, and Teixeira JP

Subjects

Cell Survival, Epithelial Cells metabolism, Humans, Oxidative Stress, Particle Size, Reactive Oxygen Species metabolism, Alveolar Epithelial Cells metabolism, DNA Damage

Abstract

High-energy industrial processes have been associated with particle release into workplace air that can adversely affect workers' health. The present study assessed the toxicity of incidental fine (PGFP) and nanoparticles (PGNP) emitted from atmospheric plasma (APS) and high-velocity oxy-fuel (HVOF) thermal spraying. Lactate dehydrogenase (LDH) release, 2-(4-nitrophenyl)-2H-5-tetrazolio]-1,3-benzene disulfonate (WST-1) metabolisation, intracellular reactive oxygen species (ROS) levels, cell cycle changes, histone H2AX phosphorylation (γ-H2AX) and DNA damage were evaluated in human alveolar epithelial cells at 24 h after exposure. Overall, HVOF particles were the most cytotoxic to human alveolar cells, with cell viability half-maximal inhibitory concentration (IC 50 ) values of 20.18 µg/cm 2 and 1.79 µg/cm 2 for PGFP and PGNP, respectively. Only the highest tested concentration of APS-PGFP caused a slight decrease in cell viability. Particle uptake, cell cycle arrest at S + G 2 /M and γ-H2AX augmentation were observed after exposure to all tested particles. However, higher levels of γ-H2AX were found in cells exposed to APS-derived particles (~16%), while cells exposed to HVOF particles exhibited increased levels of oxidative damage (~17% tail intensity) and ROS (~184%). Accordingly, APS and HVOF particles seem to exert their genotoxic effects by different mechanisms, highlighting that the health risks of these process-generated particles at industrial settings should not be underestimated.

Published

2022

234. Cytotoxic and Inflammatory Effects of Electronic and Traditional Cigarettes on Oral Gingival Cells Using a Novel Automated Smoking Instrument: An In Vitro Study.

Author

Ramenzoni LL, Schneider A, Fox SC, Meyer M, Meboldt M, Attin T, and Schmidlin PR

Abstract

Information about the potential oral health effects of vaping from electronic cigarettes (e-cigs) is still sparse and inconsistent. The purpose of this study was to compare the safety and cytotoxicity of e-cig liquid aerosols versus traditional cigarette (t-cig) smoke on human epithelial oral cells. T-cig smoke and e-cig aerosols were generated by a newly developed automated smoking instrument in order to simulate realistic user puffing behaviors. Air−liquid interface transwell cell cultures were exposed to standardized puff topography (puff duration: 2 s, puff volume: 35 mL, puff frequency: 1 puff every 60 s) of reference t-cigs or commercially available e-cigs at different air dilutions. Cell viability, morphology, and death rate were evaluated with MTT and TUNEL assays. The inflammatory cytokine gene expression of inflammatory genes was assessed by quantitative RT-PCR. E-cigs and t-cigs indicated similar adverse effects by enhancing cytotoxicity and cell death in a dose-dependent manner. E-cig aerosol and t-cig smoke treatment expressed upregulation of inflammatory cytokines up to 3.0-fold (p < 0.05). These results indicate that e-cig smoking may contribute to oral tissue−cell damage and tissue inflammation. Our approach allows the production of e-cig aerosol and t-cig smoke in order to identify harmful effects in oral tissues in vitro.

Published

2022

235. Rational deuteration of dronedarone attenuates its toxicity in human hepatic HepG2 cells.

Author

Tang LWT, Lim RYR, Venkatesan G, and Chan ECY

Abstract

Deuteration is a chemical modification strategy that has recently gained traction in drug development. The replacement of one or more hydrogen atom(s) in a drug molecule with its heavier stable isotope deuterium can enhance its metabolic stability and pharmacokinetic properties. However, it remains uninterrogated if rational deuteration at bioactivation "hot-spots" could attenuate its associated toxicological consequences. Here, our preliminary screening with benzofuran antiarrhythmic agents first revealed that dronedarone and its major metabolite N-desbutyldronedarone elicited a greater loss of viability and cytotoxicity in human hepatoma G2 (HepG2) cells as compared with amiodarone and its corresponding metabolite N-desethylamiodarone. A comparison of dronedarone and its in-house synthesized deuterated analogue (termed poyendarone) demonstrated that deuteration could attenuate its in vitro toxicity in HepG2 cells by modulating the extent of mitochondrial dysfunction, reducing the dissipation of mitochondrial membrane potential, and evoking a distinct apoptotic kinetic signature. Furthermore, although pretreatment with the CYP3A inducer rifampicin or the substitution of glucose with galactose in the growth media significantly augmented the loss of cell viability elicited by dronedarone and poyendarone, a lower loss of cell viability was consistently observed in poyendarone across all concentrations. Taken together, our preliminary investigations suggested that the rational deuteration of dronedarone at its benzofuran ring reduces aberrant cytochrome P450 3A4/5-mediated bioactivation, which attenuated its mitochondrial toxicity in human hepatic HepG2 cells., (© The Author(s) 2022. Published by Oxford University Press. All rights reserved. For Permissions, please email: journals.permissions@oup.com.)

Published

2022

236. In Vitro Assessment Reveals the Effects of Environmentally Persistent Free Radicals on the Toxicity of Photoaged Tire Wear Particles.

Author

Liu Z, Sun Y, Wang J, Li J, and Jia H

Subjects

Free Radicals chemistry, Humans, Plastics

Abstract

Tire wear particles (TWP) have been identified as one of the major sources of microplastics (MPs), and few studies have focused on their environmental behaviors and impacts. However, a thorough characteristic and toxicity assessment associated with environmentally persistent free radicals (EPFRs) on the photoaged TWP is missing. In this study, we investigated EPFRs in the process of TWP photoaging and evaluated their toxicity using in vitro bioassays. Our results showed that a total of around 1.0 × 10 17 spins/g EPFRs ( g -factors ranging 2.00308-2.00318) was formed on TWP with 60 days of light irradiation, which contained more than 29% of reactive EPFRs (r-EPFRs). Using macrophages as model cells for bioassays, TWP-associated EPFRs trigged endpoints, including the decrease of cell viability (27 to 45%) and the increase of oxidative stress response (46-93%) and inflammatory factor secretion. The enhancement of TWP toxicity with photoaging was confirmed to be attributed to the generated EPFRs combined with other TWP's chemical compositions (e.g., various metals and organics). Most importantly, the toxicity of photoaged TWP was closely correlated with the generated r-EPFRs, which induced reactive oxidant species (ROS) generation. This study provides direct evidence of toxicity on the photoaged TWP particles, revealing the potential contributions of EPFRs to the adverse effect on human health and highlighting the need for an improved understanding of the impacts of EPFRs on the risk assessment of TWP released into the environment.

Published

2022

237. In Vitro Toxicity of TiO2:SiO2 Nanocomposites with Different Photocatalytic Properties

Author

Bengalli, R, Ortelli, S, Blosi, M, Costa, A, Mantecca, P, Fiandra, L, Bengalli, Rossella, Ortelli, Simona, Blosi, Magda, Costa, Anna, Mantecca, Paride, Fiandra, Luisa, Bengalli, R, Ortelli, S, Blosi, M, Costa, A, Mantecca, P, Fiandra, L, Bengalli, Rossella, Ortelli, Simona, Blosi, Magda, Costa, Anna, Mantecca, Paride, and Fiandra, Luisa

Abstract

The enormous technological relevance of titanium dioxide (TiO2) nanoparticles (NPs) and the consequent concerns regarding potentially hazardous effects that exposure during production, use, and disposal can generate, encourage material scientists to develop and validate intrinsically safe design solution (safe-by-design). Under this perspective, the encapsulation in a silica dioxide (SiO2) matrix could be an effective strategy to improve TiO2 NPs safety, preserving photocatalytic and antibacterial properties. In this work, A549 cells were used to investigate the toxic effects of silica-encapsulated TiO2 having different ratios of TiO2 and SiO2 (1:1, 1:3, and 3:1). NPs were characterized by electron microscopy and dynamic light scattering, and cell viability, oxidative stress, morphological changes, and cell cycle alteration were evaluated. Resulting data demonstrated that NPs with lower content of SiO2 are able to induce cytotoxic effects, triggered by oxidative stress and resulting in cell necrosis and cell cycle alteration. The physicochemical properties of NPs are responsible for their toxicity. Particles with small size and high stability interact with pulmonary cells more effectively, and the different ratio among silica and titania plays a crucial role in the induced cytotoxicity. These results strengthen the need to take into account a safe(r)-by-design approach in the development of new nanomaterials for research and manufacturing.

Published

2019

238. In vitro pulmonary and vascular effects induced by different diesel exhaust particles

Author

Bengalli, R, Zerboni, A, Marchetti, S, Longhin, E, Priola, M, Camatini, M, Mantecca, P, Bengalli R., Zerboni A., Marchetti S., Longhin E., Priola M., Camatini M., Mantecca P., Bengalli, R, Zerboni, A, Marchetti, S, Longhin, E, Priola, M, Camatini, M, Mantecca, P, Bengalli R., Zerboni A., Marchetti S., Longhin E., Priola M., Camatini M., and Mantecca P.

Abstract

Diesel exhaust particles (DEP) are responsible for both respiratory and cardiovascular effects. However many questions are still unravelled and the mechanisms behind the health effects induced by the exposure to ultrafine particles (UFP) need further investigations. Furthermore, different emission sources can lead to diverse biological responses. In this perspective, here we have compared the effects of three DEPs, two standard reference materials (SRM 1650b and 2975) and one DEP directly sampled from a EuroIV vehicle without Diesel Particulate Filter (DPF). For the biological investigations, different in vitro lung models involving both epithelial and vascular endothelial cells, were used. Cell viability, oxidative stress, inflammation, DNA damage and endothelial activation markers were investigated at sub-cytotoxic DEP doses. The data obtained have shown that only DEP EuroIV, which had the major content of polycyclic aromatic hydrocarbons (PAHs) and metals, was able to induce oxidative stress, inflammation and consequent endothelial activation, as demonstrated by the expression of adhesion molecules (ICAM-1 and VCAM-1) and the release of inflammatory markers (IL-8) from endothelial cells. Standard reference materials were not effective under our experimental conditions. These data suggest that oxidative stress, endothelial activation and systemic inflammatory cytokines release are crucial events after DEP exposure and that the source of DEP emission, responsible of the particle chemical fingerprint, may have a key role in the resulting adverse biological outcomes.

Published

2019

239. Chemical composition and toxicity of emissions from burning five vegetation types of Western Australia under experimental combustion conditions

Author

Dong, T T Trang and Dong, T T Trang

Abstract

This study investigated the emission factors (EFs) for inorganic gases (CO2, CO, SO2, NO and NO2), carbonyls (formaldehyde, acetaldehyde, acetone, propionaldehyde, butyraldehyde and benzaldehyde), volatile organic compounds (VOCs) and particulate matter (PM2.5 and PM10) from laboratory-based fires of vegetation from five typical vegetation types of Western Australia. Species burnt were three grasslands (Spinifex represented by Triodia basedowii, Kimberley grass represented by Sehima nervosum and Heteropogon contortus, and an invasive grass represented by Ehrharta calycina (Veldt grass)), Banksia woodland and Jarrah forest under different combustion conditions. Chemical composition (water-soluble metals and polycyclic aromatic hydrocarbons – PAHs) and in vitro toxicity of PM2.5 were also measured. Vegetation samples were burnt in a ceramic chamber in varying combustion conditions altered by controlling the vegetation moisture content (<10%, 12–16% and 20–25%) and the air flow rate (0, 1.25 and 2.94 m.s-1). Burns of woodland (Banksia) and forest (Jarrah) had significantly higher EFs for CO, SO2 and PM2.5 compared with those from grassland (Spinifex). Emissions of temperate grass (Veldt) fires were significantly different from those of the tropical grass (Spinifex and Kimberley grasses), with lower EFCO2 and higher EFs for CO, carbonyls and PM2.5. EFs for SO2, NO and NO2 were variable between different vegetation types, indicating variation in the nitrogen and sulphur content of the fuels. The EFs for most carbonyls were similar between most vegetation types, with the exception of Veldt grass. Functions which may be useful to predict emissions of infrequently measured carbonyls (acetaldehyde, acetone and propionaldehyde) from the EF for formaldehyde, a commonly measured and reported substance, were also proposed. Fifteen VOCs were identified in the smoke, but concentrations were too low to be quantified. Benzene, toluene, styrene and indene were the most frequently det

Published

2019

240. Cytotoxicity against fish and mammalian cell lines and endocrine activity of the mycotoxins beauvericin, deoxynivalenol and ochratoxin-A

Author

Ministerio de Economía y Competitividad (España), Valdehita Torija, Ana [0000-0003-2120-6924], Navas, José María [0000-0002-7644-8499], Fernández-Cruz, M. L. [0000-0001-5988-1939], García-Herranz, V, Valdehita Torija, Ana, Navas, José María, Fernández-Cruz, M. L., Ministerio de Economía y Competitividad (España), Valdehita Torija, Ana [0000-0003-2120-6924], Navas, José María [0000-0002-7644-8499], Fernández-Cruz, M. L. [0000-0001-5988-1939], García-Herranz, V, Valdehita Torija, Ana, Navas, José María, and Fernández-Cruz, M. L.

Abstract

The toxicity of mycotoxins is well recognized in mammals, but their effects on fish have received less attention. Moreover, in the last years several studies have reported that some mycotoxins may act as endocrine disruptors. The aim of this study was to determine the cytotoxic effects and endocrine activities of three mycotoxins: beauvericin, deoxynivalenol and ochratoxin-A. Cytotoxicity in two fish hepatoma and one mammalian hepatoma cell lines was determined by the AlamarBlue, Neutral Red Uptake and CFDA-AM assays. For the assessment of androgenic, estrogenic and thyroidal agonistic/antagonistic effects three cell lines stably expressing luciferase as reporter gene under the control of hormone receptors were used. Results showed that both fish and mammalian cell lines were very sensitive to the mycotoxins tested. OTA was the least toxic mycotoxin and DON and BEA showed similar acute toxicity. None of the three mycotoxins tested presented agonistic effects at the receptors studied, but all of them showed strong antagonistic effect at the thyroid receptor. BEA showed a weak antagonistic effect at the androgen receptor and OTA produced a biphasic dose-response curve at the estrogen receptor. The data obtained in this work are of high interest for aquaculture industries and for regulators.

Published

2019

241. Mannitol Polymorphs as Carrier in DPIs Formulations: Isolation Characterization and Performance.

Author

Altay Benetti, Ayça, Bianchera, Annalisa, Buttini, Francesca, Bertocchi, Laura, and Bettini, Ruggero

Subjects

*MANNITOL, *PARTICULATE matter, *LUNGS, *DRUG carriers, *ALBUTEROL, *CELL lines

Abstract

The search for best performing carriers for dry powder inhalers is getting a great deal of interest to overcome the limitations posed by lactose. The aerosolization of adhesive mixtures between a carrier and a micronized drug is strongly influenced by the carrier solid-state properties. This work aimed at crystallizing kinetically stable D-mannitol polymorphs and at investigating their aerosolization performance when used in adhesive mixtures with two model drugs (salbutamol sulphate, SS, and budesonide, BUD) using a median and median/high resistance inhaler. A further goal was to assess in vitro the cytocompatibility of the produced polymer-doped mannitol polymorphs toward two lung epithelial cell lines. Kinetically stable (up to 12 months under accelerate conditions) α, and δ mannitol forms were crystallized in the presence of 2% w/w PVA and 1% w/w PVP respectively. These solid phases were compared with the β form and lactose as references. The solid-state properties of crystallized mannitol significantly affected aerosolization behavior, with the δ form affording the worst fine particle fraction with both the hydrophilic (9.3 and 6.5%) and the lipophilic (19.6 and 32%) model drugs, while α and β forms behaved in the same manner (11–13% for SS; 53–58% for BUD) and better than lactose (8 and 13% for SS; 26 and 39% for BUD). Recrystallized mannitol, but also PVA and PVP, proved to be safe excipients toward lung cell lines. We concluded that, also for mannitol, the physicochemical properties stemming from different crystal structures represent a tool for modulating carrier-drug interaction and, in turn, aerosolization performance. [ABSTRACT FROM AUTHOR]

Published

2021

242. Deep eutectic systems from betaine and polyols – Physicochemical and toxicological properties.

Author

Rodrigues, Liliana A., Cardeira, Martim, Leonardo, Inês C., Gaspar, Frédéric B., Radojčić Redovniković, Ivana, Duarte, Ana Rita C., Paiva, Alexandre, and Matias, Ana A.

Subjects

*PROPYLENE glycols, *EUTECTIC reactions, *ETHYLENE glycol, *WHEAT, *BETAINE, *HYDROGEN bonding, *POLYOLS, *WATER temperature

Abstract

[Display omitted] • DES were prepared from mixtures of betaine, glycerol, propylene glycol, ethylene glycol, and water. • DES properties could be tuned not only through the hydrogen bond donor, but also by temperature, and water content. • DES presented different toxicological responses towards different organisms. • Generally, the toxicity profile of DES was low and decreased with increasing water content. The tailor-made versatility of deep eutectic systems (DES) has opened promising future perspectives for their applications in industry, to complement or even replace some of the already existing processes. Although there has been an active and considerable effort by the scientific community to characterize these systems, their toxicity towards different living organisms has not yet been thoroughly investigated. In this work, different mixtures of betaine with glycerol, propylene glycol, ethylene glycol, and their mixtures with water, were prepared and characterized in terms of density, viscosity, and polarity. Additionally, DES effects were also evaluated on a human intestinal epithelial cell model (Caco-2), towards a Gram-positive (Staphylococcus aureus) and a Gram-negative (Escherichia coli) bacterium, and on wheat (Triticum aestivum) seeds. Results showed that the physicochemical properties of the DES tested, namely density and viscosity, could be tuned not only through the hydrogen bond donor, but also by changing temperature or the water content. Polarity was also considerably affected by the water content of the system. Additionally, although DES presented different responses towards different organisms, generally, the systems presented a low toxicity profile, which could be substantially reduced by increasing their water content. These findings suggest that the DES studied can be minimally toxic, with easily tunable properties, which reinforces the prospect of using this kind of systems in the field of green technologies. [ABSTRACT FROM AUTHOR]

Published

2021

243. Silica-coated manganite and Mn-based ferrite nanoparticles: a comparative study focused on cytotoxicity

Author

Kaman, Ondřej, Dědourková, Tereza, Koktan, Jakub, Kuličková, Jarmila, Maryško, Miroslav, Veverka, Pavel, Havelek, Radim, Královec, Karel, Turnovcová, Karolína, Jendelová, Pavla, Schröfel, Adam, and Svoboda, Ladislav

Published

2016

244. Sugar-Mediated Green Synthesis of Silver Selenide Semiconductor Nanocrystals under Ultrasound Irradiation

Author

Alexis Debut, Si Amar Dahoumane, Thibault Terencio, Lupe Mendoza, Clayton Jeffryes, Edward E. Ávila, Alex Gavilanes, Karla Vizuete, Marbel Torres Arias, and Daniela Armijo García

Subjects

Salmonella typhimurium, Staphylococcus aureus, Materials science, Cell Survival, Scanning electron microscope, Metal Nanoparticles, Pharmaceutical Science, Nanoparticle, Antineoplastic Agents, in vitro toxicity, semiconductors, Selenious Acid, Article, fructose, Analytical Chemistry, Sonochemistry, Nanomaterials, lcsh:QD241-441, Selenous acid, chemistry.chemical_compound, lcsh:Organic chemistry, Polysaccharides, Cell Line, Tumor, Selenide, Drug Discovery, Escherichia coli, Humans, Physical and Theoretical Chemistry, Selenium Compounds, Aqueous solution, green chemistry, starch, Organic Chemistry, technology, industry, and agriculture, Silver Compounds, Green Chemistry Technology, Anti-Bacterial Agents, Silver nitrate, chemistry, Chemistry (miscellaneous), Pseudomonas aeruginosa, Silver Nitrate, silver selenide, Molecular Medicine, nanoparticles, Sugars, sonochemistry, Nuclear chemistry

Abstract

Silver selenide (Ag2Se) is a promising nanomaterial due to its outstanding optoelectronic properties and countless bio-applications. To the best of our knowledge, we report, for the first time, a simple and easy method for the ultrasound-assisted synthesis of Ag2Se nanoparticles (NPs) by mixing aqueous solutions of silver nitrate (AgNO3) and selenous acid (H2SeO3) that act as Ag and Se sources, respectively, in the presence of dissolved fructose and starch that act as reducing and stabilizing agents, respectively. The concentrations of mono- and polysaccharides were screened to determine their effect on the size, shape and colloidal stability of the as-synthesized Ag2Se NPs which, in turn, impact the optical properties of these NPs. The morphology of the as-synthesized Ag2Se NPs was characterized by transmission electron microscopy (TEM) and both &alpha, and &beta, phases of Ag2Se were determined by X-ray diffraction (XRD). The optical properties of Ag2Se were studied using UV&ndash, Vis spectroscopy and its elemental composition was determined non-destructively using scanning electron microscopy&ndash, energy-dispersive spectroscopy (SEM&ndash, EDS). The biological activity of the Ag2Se NPs was assessed using cytotoxic and bactericidal approaches. Our findings pave the way to the cost-effective, fast and scalable production of valuable Ag2Se NPs that may be utilized in numerous fields.

Published

2020

245. CYTOTOXICITY OF FLUORESCENT BENZIMIDAZOLE CORE COMPOUNDS

Author

Krajeski, Daiane Metz, Mota, Chaiana, Schrekker, Henri Stephan, Perin, Nataša, Hranjec, Marijana, Ziulkoski, Ana Luisa, and Linden, Rafael

Subjects

in vitro toxicity, cell viability, MTT, benzimidazole analogs

Abstract

Background: Benzimidazoles are heterocyclic aromatic organic compounds, which consist of the fusion of benzene and imidazole. Various biological actions have been identified for this class of compounds, such as antineoplastic, antimicrobial and anti-inflammatory. The in vitro cellular toxicity of biologically active compounds is a preclinical approach that definesthe therapeutic window ofdrugs. Therefore, we evaluated the in vitro cytotoxicity of six fluorescent benzimidazole core compounds (NB2, NB5, NB6, NB7, NB8, NB9), using a mitochondrial assay based on the reduction of MTT. Methods: VERO cells were cultured in DMEM supplemented with 10% fetal bovine serum (conventional medium) at 37°C in a humid atmosphere with 5% CO2. Cell cultures at 80% confluence were exposed for 72h to 0.001, 0.01, 0.1, 1.0, 10 and 100 μM of each of the six compounds. Untreated cells maintained in conventional medium were used as negative control (100% viable cells). After the incubation time, the MTT assay was performed and the cytotoxic concentrationfor 50% of the cells (CC50) was calculated from the polynomial equation of the dose-response pattern. Results: All concentration versus cell viability curves obtained exhibit a concentration dependent profile. Taking into consideration the maximum concentration evaluated (100 μM) and the CC50 of each compound, NB5 (97%), NB7 (100%) and NB8 (100%) showed the highest cytotoxicity’s. NB2 and NB9 showed 54% and 72% of cytotoxicity, respectively, while NB6 was the least toxic compound with around 75% of viable cells remaining. The CC50 concentrations of the NB compounds were between 20 μM (NB8) and 2.35μM (NB6). Interestingly, increased mitochondrial activities of up to 25% were determined below 1.0 μM. Conclusions: This study demonstrates that the benzimidazole compound NB6 is the least toxic one and may be tested in a broader therapeutic window to evaluate its biological action like antiviral, antibacterial or antifungal.

Published

2019

246. Study on cytotoxicity of devolopmental antimicrobial substances

Author

Zádrapová, Marie, Maixnerová, Jana, and Bárta, Pavel

Subjects

cytotoxicity, životnost buněk, inhibition of metabolism, in vitro toxicity, hepatocyty, in vitro toxicita, hepatocytes, cytotoxicita, inhibice metabolismu, cell viability

Published

2019

247. L-glutamic acid-g-p(HEMA) polimerik nanopartiküllerinin sentezi, karakterizasyonu, in vitro ve in vivo toksisite potensiyeli

Author

Bakan, Nafiye Buket, Karabay Yavaşoğlu, Nefise Ülkü, Biyoloji Anabilim Dalı, Karabay Yavaşoğlu, N.Ülkü, and Fen Bilimleri Enstitüsü

Subjects

Polymeric Nanoparticle, Polimerik Nanopartikül, p(HEMA), Biodistribution, Cytotoxicity, Biyodağılım, Genotoxicity, İn Vitro Toxicity, Biology, İn Vitro Toksisite, Biyoloji

Abstract

Nanomateryaller fiziksel ve kimyasal olarak modifiye edilebilen malzemeler olup, tıp, biyomedikal, endüstri gibi birçok alanda yaygın olarak kullanımlarıyla, son yıllarda büyük ölçüde araştırmalara konu olmuştur. Sürfaktansız emülsiyon polimerizasyon yöntemiyle elde edilen p(HEMA) ile L-glutamik asit graftlama tekniği ile sentezlenmiştir. Polimerik nanopartiküllün karakterizasyon analizleri, boyut ve morfolojik özelliklerini incelemek amacıyla SEM (Scanning Electron Microscopy) görüntülemesi, polar sıvılar içerisindeki davranışlarını belirlemek amacıyla ZETA boyut- potansiyel analizi, yüzey topografyasını görüntülemek amacıyla AFM (Atomik Kuvvet Mikroskobu) analizi ve yapıdaki bileşenlerin yüzey kimyası ile etkileşimlerini belirlemek amacıyla FTIR Absorbsiyon Spektroskopisi gerçekleştirilmiştir. Karakterizasyon analiz sonuçlarına göre 194.6 nm boyutunda olan L-glutamik asit-g-p(HEMA), -18 Mv yüzey yüküne sahiptir. Elde edilen polimerik nanopartikülün in vitro ve in vivo deneysel yöntemlerle toksisitesi belirlenmiştir. L-glutamik asit-g-p(HEMA)'nın, 16HBE (Human bronchial epithelial cell line) ve THP-1 (human monocytic cell line) hücre hatları üzerinde üzerinde WST-1 ve LDH testleri ile sitotoksik etki göstermediği, mutajenik potansiyelin belirlenmesi amacıyla Salmonella typhimurium suşları üzerinde gerçekleştirilen Salmonella/AMES testi sonucunda mutajenik olmadığı saptanmıştır. Genotoksik potansiyelini belirlemek amacıyla 16HBE ve THP-1 hücre hatları ile yapılan COMET testi, ve in vivo kemik iliği ile mikronukleus testi sonucunda genotoksik etki göstermediği belirlenmiştir. 16HBE hücre hattında hücre migrasyon testi gerçekleştirilmiş kapanma yüzdesi %21 olarak belirlenmiştir. HET-CAM testi ile uygulanan konsantrasyonlarda irritasyon potansiyeli ve MIC yöntemi ile antimikrobiyal etkinliği ortaya konulmuştur. In vivo tek doz akut toksisite testi ile LD50 değeri ≥ 2000 mg/kg olarak belirlenmiş, 28 gün tekrarlı doz toksisite (subakut) çalışması sonucunda hayvan ve organ ağırlık verileriyle birlikte biyokimyasal veriler sağlanmış, histopatolojik incelemeler gerçekleştirilmiş ve herhangi bir toksik bulguya rastlanmamıştır. Polimerik nanopartikülün vücut içerisinde biyodağılımı in vivo görüntüleme sistemi olan IVIS spektrum ile ortaya konmuştur. Sonuç olarak sentezlediğimiz ve karakterize ettiğimiz polimerik nanopartikül olan L-glutamik asit-g-p(HEMA)'nın biyouyumlu olduğu ve ilaç taşıma sistemi olarak kullanılabilme potansiyeli bulunduğu ortaya konmuştur., Nanomaterials can be physically and chemically modified and have been used commonly in recent years with their widespread use in many areas as medicine, biomedical and industry. p(HEMA) was obtained with surfactant free emulsion polymerization method and it was synthesized with L-glutamic acid by grafting technique. Characterization analysis of polymeric nanoparticles were investigated by SEM (Scanning Electron Microscopy) imaging to determine their size and morphological characteristics, ZETA size-potential analysis to determine their behavior in polar liquids, AFM (Atomic Force Microscopy) analysis to display surface topography and their interactions with surface chemistry by FTIR Absorption Spectroscopy. According to the results of characterization analysis, L-glutamic acid-g-p (HEMA) has 194.6 nm size and -18 Mv negative surface value. The toxicity of polymeric nanoparticle was determined with in vitro and in vivo assays. L-glutamic acid-g-p (HEMA) has no cytotoxic effect on 16HBE (Human bronchial epithelial cell line) and THP-1 (human monocytic cell line) cell lines with WST-1 and LDH tests and in order to determine the mutagenic potential on Salmonella typhimurium strains which was not showed mutagenic effect with Salmonella/AMES test. In order to determine genotoxic potential, it has been identified that there is no genotoxic effect with COMET test on 16HBE and THP-1 cell lines and in vivo micronucleus test on bone marrow. Cell migration test was performed on 16HBE cell line and the percent closure rate was determined as 21%. The irritation potential was obtained with applied concentration by HET-CAM test and antimicrobial activity were determined with MIC method. The LD50 value was determined as ≥ 2000 mg / kg by the in vivo single dose acute toxicity test, also biochemical data and histopathological investigation were obtained with the animal and organ weight data as a nontoxic result of the 28 days repeated dose toxicity (subacute) study. The biodistribution of the polymeric nanoparticle in the body was demonstrated by IVIS spectrum which is in vivo imaging system. As a result, L-glutamic acid-g-p (HEMA), a polymeric nanoparticle which was synthesized and characterized by us, has been found to be biocompatible and has the potential to be used as a drug delivery system.

Published

2019

248. Usefulness of fish cell lines for the initial characterization of toxicity and cellular fate of graphene-related materials (carbon nanofibers and graphene oxide)

Author

María Luisa Fernández-Cruz, José María Navas, Cesar Merino, and Judit Kalman

Subjects

Neutral red, Environmental Engineering, Cell Survival, Health, Toxicology and Mutagenesis, 0208 environmental biotechnology, Nanofibers, 02 engineering and technology, 010501 environmental sciences, Ecotoxicology, 01 natural sciences, Cell Line, chemistry.chemical_compound, Fish hepatocytes, Liver Neoplasms, Experimental, Microscopy, Electron, Transmission, Carbon nanofibers, Toxicity Tests, In vitro toxicity, Environmental Chemistry, Animals, Viability assay, Cytotoxicity, 0105 earth and related environmental sciences, Graphene oxide, Dose-Response Relationship, Drug, Carbon nanofiber, Vesicle, Macrophages, Public Health, Environmental and Occupational Health, Fishes, General Medicine, General Chemistry, Fish macrophages, Pollution, 020801 environmental engineering, Mitochondria, chemistry, Cytoplasm, Cell culture, Toxicity, Biophysics, Hepatocytes, Graphite, Lysosomes

Abstract

Graphene-related materials (GRMs) are one of the most attractive materials from an application perspective, consequently their release into aquatic environments is highly likely. In the present work, the potential of fish hepatocytes (topminnow fish hepatoma cell line, PLHC-1) and macrophages (carp leukocyte cell line, CLC) to study the toxicity and intracellular fate of helical-ribbon carbon nanofibers (CNFs) and graphene oxide (GO) used in a variety of intermediate industrial products was evaluated, allowing a first ranking of GRMs according to their cytotoxicity. Cells were exposed to a concentration range of 0–200 μg ml−1 of GRMs for 24 and 72 h and cell viability was assessed by measuring mitochondrial activity (AlamarBlue assay), plasma membrane integrity (5-carboxyfluorescein diacetate-acetoxymethyl ester assay) and lysosomal function (neutral red uptake assay). Results showed that both the cell type and the choice of endpoint determined the toxicity of GRMs. In both cell lines, CNFs appeared to have higher toxicity than GO and the highest degree of graphitization in fibers was associated with lower toxicity. Transmission electron microscopy revealed that CNFs were taken up into membrane-bound compartments of PLHC-1 cells in a size-independent manner, whereas in CLC, longer CNFs were encountered free in the cytoplasm and only the shorter CNFs were localized in membrane-surrounded vesicles. GO sheets were present within vesicles as well as free in the cytoplasm of both cell types. These findings contribute to the understanding of the toxicity and behaviour of these GRMs in living systems, therefore aiding in designing safer materials for the environment.

Published

2019

249. Partial In Vitro Digestion of Active Gliadin-Related Peptides in Celiac Disease.

Author

Cornell, Hugh

Abstract

Peptides corresponding to residues 75–86 (RPQQPYPQPQPQ) and 75–85 of the A-gliadin structure, which were shown to be active in an animal model of celiac disease, were digested in vitro with small intestinal mucosa from children with celiac disease in remission and with mucosa from normal children. The products of digestion were separated into two fractions by gel permeation chromatography. Undigested residues (M r > 400 fraction) from both peptides contained mainly glutamine, proline, and tyrosine, while the digested materials (M r < 400 fraction) contained mainly proline, glutamine and arginine. Much larger amounts of undigested peptides were obtained from digestion with celiac mucosa than from normal mucosa. The results with peptide 75–86 indicated that the octapeptide 77–84 (QQPYPQPQ) was the main residual component and this peptide was shown to be active in the assay. Peptide 77–84 was also obtained as a residue from digestion of peptide 75–85, together with heptapeptide 77–83. The results lend further support for a primary mucosal defect in celiac disease and indicate that residual peptides in the small intestine of patients with the disease still retain appreciable toxicity. [ABSTRACT FROM AUTHOR]

Published

1998

250. Erwinia soft rot resistance of potato cultivars expressing antimicrobial peptide tachyplesin I.

Author

Allefs, Sjefke, Jong, Eliza, Florack, Dion, Hoogendoorn, Coosje, and Stiekema, Willem

Abstract

Tachyplesin I is a 2.3 kDa antimicrobial peptide isolated from Southeast Asian horseshoe crabs. Bacterial suspensions containing 1×10 colony-forming units/ml of six isolates of pectolytic Erwinia spp., the causal pathogens of potato soft rot and blackleg, were killed in vitro by 1.4 to 11.1 μg/ml of tachyplesin I. In an attempt to enhance resistance to Erwinia spp., each of the potato cultivars Bintje, Karnico and Kondor were transformed with two gene constructs encoding different precursor tachyplesin I proteins under the control of a cauliflower mosaic virus 35S promotor. Northern and western blot analysis showed that the tachyplesin I gene was expressed in transgenic plants. Small tubers of 17 transgenic clones were screened twice for soft rot resistance to Erwinia carotovora ssp. atroseptica. Under aerobic or anaerobic conditions, transgenic clones showed slightly less rot than control tubers. [ABSTRACT FROM AUTHOR]

Published

1996