Your search keyword '"Francesconi K"' showing total 5 results

1. Toxicity of three types of arsenolipids: species-specific effects in Caenorhabditis elegans.

Author

Bornhorst J, Ebert F, Meyer S, Ziemann V, Xiong C, Guttenberger N, Raab A, Baesler J, Aschner M, Feldmann J, Francesconi K, Raber G, and Schwerdtle T

Subjects

Animals, Caenorhabditis elegans drug effects, Arsenic toxicity, Caenorhabditis elegans growth & development, Fatty Acids toxicity, Hydrocarbons toxicity, Triglycerides toxicity

Abstract

Although fish and seafood are well known for their nutritional benefits, they contain contaminants that might affect human health. Organic lipid-soluble arsenic species, so called arsenolipids, belong to the emerging contaminants in these food items; their toxicity has yet to be systematically studied. Here, we apply the in vivo model Caenorhabditis elegans to assess the effects of two arsenic-containing hydrocarbons (AsHC), a saturated arsenic-containing fatty acid (AsFA), and an arsenic-containing triacylglyceride (AsTAG) in a whole organism. Although all arsenolipids were highly bioavailable in Caenorhabditis elegans, only the AsHCs were substantially metabolized to thioxylated or shortened metabolic products and induced significant toxicity, affecting both survival and development. Furthermore, the AsHCs were several fold more potent as compared to the toxic reference arsenite. This study clearly indicates the need for a full hazard identification of subclasses of arsenolipids to assess whether they pose a risk to human health.

Published

2020

2. Arsenolipids exert less toxicity in a human neuron astrocyte co-culture as compared to the respective monocultures.

Author

Witt B, Bornhorst J, Mitze H, Ebert F, Meyer S, Francesconi KA, and Schwerdtle T

Subjects

Arsenic Poisoning metabolism, Arsenicals metabolism, Astrocytes cytology, Astrocytes metabolism, Cell Culture Techniques, Cell Line, Cell Survival drug effects, Coculture Techniques, Humans, Lipid Metabolism, Neurons cytology, Neurons drug effects, Neurons metabolism, Arsenic Poisoning etiology, Arsenicals chemistry, Astrocytes drug effects, Lipids chemistry, Lipids toxicity

Abstract

Arsenic-containing hydrocarbons (AsHCs), natural products found in seafood, have recently been shown to exert toxic effects in human neurons. In this study we assessed the toxicity of three AsHCs in cultured human astrocytes. Due to the high cellular accessibility and substantial toxicity observed astrocytes were identified as further potential brain target cells for arsenolipids. Thereby, the AsHCs exerted a 5-19-fold higher cytotoxicity in astrocytes as compared to arsenite. Next we compared the toxicity of the arsenicals in a co-culture model of the respective human astrocytes and neurons. Notably the AsHCs did not show any substantial toxic effects in the co-culture, while arsenite did. The arsenic accessibility studies indicated that in the co-culture astrocytes protect neurons against cellular arsenic accumulation especially after incubation with arsenolipids. In summary, these data underline the importance of the glial-neuron interaction when assessing the in vitro neurotoxicity of new unclassified metal species.

Published

2017

3. In vitro toxicological characterisation of arsenic-containing fatty acids and three of their metabolites.

Author

Meyer S, Raber G, Ebert F, Leffers L, Müller SM, Taleshi MS, Francesconi KA, and Schwerdtle T

Abstract

Arsenic-containing fatty acids are a group of fat-soluble arsenic species (arsenolipids) which are present in marine fish and other seafood. Recently, it has been shown that arsenic-containing hydrocarbons, another group of arsenolipids, exert toxicity in similar concentrations comparable to arsenite although the toxic modes of action differ. Hence, a risk assessment of arsenolipids is urgently needed. In this study the cellular toxicity of a saturated (AsFA 362) and an unsaturated (AsFA 388) arsenic-containing fatty acid and three of their proposed metabolites (DMA V , DMAPr and thio-DMAPr) were investigated in human liver cells (HepG2). Even though both arsenic-containing fatty acids were less toxic as compared to arsenic-containing hydrocarbons and arsenite, significant effects were observable at μM concentrations. DMA V causes effects in a similar concentration range and it could be seen that it is metabolised to its highly toxic thio analogue thio-DMA V in HepG2 cells. Nevertheless, DMAPr and thio-DMAPr did not exert any cytotoxicity. In summary, our data indicate that risks to human health related to the presence of arsenic-containing fatty acids in marine food cannot be excluded. This stresses the need for a full in vitro and in vivo toxicological characterisation of these arsenolipids.

Published

2015

4. Arsenic-containing hydrocarbons are toxic in the in vivo model Drosophila melanogaster.

Author

Meyer S, Schulz J, Jeibmann A, Taleshi MS, Ebert F, Francesconi KA, and Schwerdtle T

Subjects

Animals, Arsenic chemistry, Female, Hydrocarbons chemistry, Life Cycle Stages drug effects, Male, Manganese, Models, Biological, Arsenic toxicity, Drosophila melanogaster drug effects, Hydrocarbons toxicity

Abstract

Arsenic-containing hydrocarbons (AsHC) constitute one group of arsenolipids that have been identified in seafood. In this first in vivo toxicity study for AsHCs, we show that AsHCs exert toxic effects in Drosophila melanogaster in a concentration range similar to that of arsenite. In contrast to arsenite, however, AsHCs cause developmental toxicity in the late developmental stages of Drosophila melanogaster. This work illustrates the need for a full characterisation of the toxicity of AsHCs in experimental animals to finally assess the risk to human health related to the presence of arsenolipids in seafood.

Published

2014

5. In vitro toxicological characterisation of three arsenic-containing hydrocarbons.

Author

Meyer S, Matissek M, Müller SM, Taleshi MS, Ebert F, Francesconi KA, and Schwerdtle T

Subjects

Adenosine Triphosphate metabolism, Arsenic chemistry, Arsenic pharmacokinetics, Biological Availability, Caspase 3 metabolism, Cell Line, DNA Damage, Humans, Hydrocarbons chemistry, Hydrocarbons pharmacokinetics, In Vitro Techniques, L-Lactate Dehydrogenase metabolism, Tandem Mass Spectrometry, Arsenic toxicity, Hydrocarbons toxicity

Abstract

Arsenic-containing hydrocarbons are one group of fat-soluble organic arsenic compounds (arsenolipids) found in marine fish and other seafood. A risk assessment of arsenolipids is urgently needed, but has not been possible because of the total lack of toxicological data. In this study the cellular toxicity of three arsenic-containing hydrocarbons was investigated in cultured human bladder (UROtsa) and liver (HepG2) cells. Cytotoxicity of the arsenic-containing hydrocarbons was comparable to that of arsenite, which was applied as the toxic reference arsenical. A large cellular accumulation of arsenic, as measured by ICP-MS/MS, was observed after incubation of both cell lines with the arsenolipids. Moreover, the toxic mode of action shown by the three arsenic-containing hydrocarbons seemed to differ from that observed for arsenite. Evidence suggests that the high cytotoxic potential of the lipophilic arsenicals results from a decrease in the cellular energy level. This first in vitro based risk assessment cannot exclude a risk to human health related to the presence of arsenolipids in seafood, and indicates the urgent need for further toxicity studies in experimental animals to fully assess this possible risk.

Published

2014