Your search keyword '"von Stedingk, H"' showing total 30 results

1. Cyclophosphamide exposure assessed with the biomarker phosphoramide mustard-hemoglobin in breast cancer patients: The TailorDose I study

Author

Gernaat, S. A. M., von Stedingk, H., Hassan, M., Nilsson, H. P., Rodriguez-Wallberg, K. A., Hedayati, E., and Rydberg, P.

Published

2021

2. Testing the Effect of Relative Pollen Productivity on the REVEALS Model: A Validated Reconstruction of Europe-Wide Holocene Vegetation

Author

Serge, M., primary, Mazier, F., additional, Fyfe, R., additional, Gaillard, M.-J., additional, Klein, T., additional, Lagnoux, A., additional, Galop, D., additional, Githumbi, E., additional, Mindrescu, M., additional, Nielsen, A., additional, Trondman, A.-K., additional, Poska, A., additional, Sugita, S., additional, Woodbridge, J., additional, Abel-Schaad, D., additional, Åkesson, C., additional, Alenius, T., additional, Ammann, B., additional, Andersen, S., additional, Anderson, R., additional, Andrič, M., additional, Balakauskas, L., additional, Barnekow, L., additional, Batalova, V., additional, Bergman, J., additional, Birks, H., additional, Björkman, L., additional, Bjune, A., additional, Borisova, O., additional, Broothaerts, N., additional, Carrion, J., additional, Caseldine, C., additional, Christiansen, J., additional, Cui, Q., additional, Currás, A., additional, Czerwiński, S., additional, David, R., additional, Davies, A., additional, De Jong, R., additional, Di Rita, F., additional, Dietre, B., additional, Dörfler, W., additional, Doyen, E., additional, Edwards, K., additional, Ejarque, A., additional, Endtmann, E., additional, Etienne, D., additional, Faure, E., additional, Feeser, I., additional, Feurdean, A., additional, Fischer, E., additional, Fletcher, W., additional, Franco-Múgica, F., additional, Fredh, E., additional, Froyd, C., additional, Garcés-Pastor, S., additional, García-Moreiras, I., additional, Gauthier, E., additional, Gil-Romera, G., additional, González-Sampériz, P., additional, Grant, M., additional, Grindean, R., additional, Haas, J., additional, Hannon, G., additional, Heather, A.-J., additional, Heikkilä, M., additional, Hjelle, K., additional, Jahns, S., additional, Jasiunas, N., additional, Jiménez-Moreno, G., additional, Jouffroy-Bapicot, I., additional, Kabailienė, M., additional, Kamerling, I., additional, Kangur, M., additional, Karpińska-Kołaczek, M., additional, Kasianova, A., additional, Kołaczek, P., additional, Lagerås, P., additional, Latalowa, M., additional, Lechterbeck, J., additional, Leroyer, C., additional, Leydet, M., additional, Lindbladh, M., additional, Lisitsyna, O., additional, López-Sáez, J.-A., additional, Lowe, John, additional, Luelmo-Lautenschlaeger, R., additional, Lukanina, E., additional, Macijauskaitė, L., additional, Magri, D., additional, Marguerie, D., additional, Marquer, L., additional, Martinez-Cortizas, A., additional, Mehl, I., additional, Mesa-Fernández, J., additional, Mighall, T., additional, Miola, A., additional, Miras, Y., additional, Morales-Molino, C., additional, Mrotzek, A., additional, Sobrino, C., additional, Odgaard, B., additional, Ozola, I., additional, Pérez-Díaz, S., additional, Pérez-Obiol, R., additional, Poggi, C., additional, Rego, P., additional, Ramos-Román, M., additional, Rasmussen, P., additional, Reille, M., additional, Rösch, M., additional, Ruffaldi, P., additional, Goni, M., additional, Savukynienė, N., additional, Schröder, T., additional, Schult, M., additional, Segerström, U., additional, Seppä, H., additional, Vives, G., additional, Shumilovskikh, L., additional, Smettan, H., additional, Stancikaite, M., additional, Stevenson, A., additional, Stivrins, N., additional, Tantau, I., additional, Theuerkauf, M., additional, Tonkov, S., additional, van der Knaap, W., additional, van Leeuwen, J., additional, Vecmane, E., additional, Verstraeten, G., additional, Veski, S., additional, Voigt, R., additional, Von Stedingk, H., additional, Waller, M., additional, Wiethold, J., additional, Willis, K., additional, Wolters, S., additional, and Zernitskaya, V., additional

Published

2023

3. Testing the Effect of Relative Pollen Productivity on the REVEALS Model : A Validated Reconstruction of Europe-Wide Holocene Vegetation

Author

Serge, M. A., Mazier, F., Fyfe, R., Gaillard, Marie-José, Klein, T., Lagnoux, A., Galop, D., Githumbi, Esther, Mindrescu, M., Nielsen, A. B., Trondman, Anna-Kari, Poska, A., Sugita, S., Woodbridge, J., Abel-Schaad, D., Åkesson, C., Alenius, T., Ammann, B., Andersen, S. T., Scott Anderson, R., Andric, M., Balakauskas, L., Barnekow, L., Batalova, V., Bergman, J., Birks, H. John B., Björkman, L., Bjune, A. E., Borisova, O., Broothaerts, N., Carrion, J., Caseldine, C., Christiansen, J., Cui, Q., Curras, A., Czerwinski, S., David, R., Davies, A. L., De Jong, R., Di Rita, F., Dietre, B., Doerfler, W., Doyen, E., Edwards, K. J., Ejarque, A., Endtmann, E., Etienne, D., Faure, E., Feeser, I., Feurdean, A., Fischer, E., Fletcher, W., Franco-Mugica, F., Fredh, E. D., Froyd, C., Garces-Pastor, S., Garcia-Moreiras, I., Gauthier, E., Gil-Romera, G., Gonzalez-Samperiz, P., Grant, M. J., Grindean, R., Haas, J. N., Hannon, G., Heather, A. -J, Heikkilae, M., Hjelle, K., Jahns, S., Jasiunas, N., Jimenez-Moreno, G., Jouffroy-Bapicot, I., Kabailiene, M., Kamerling, I. M., Kangur, M., Karpinska-Kolaczek, M., Kasianova, A., Kolaczek, P., Lageras, P., Latalowa, M., Lechterbeck, J., Leroyer, C., Leydet, M., Lindbladh, M., Lisitsyna, O., Lopez-Saez, J. -A, Lowe, John, Luelmo-Lautenschlaeger, R., Lukanina, E., Macijauskaite, L., Magri, D., Marguerie, D., Marquer, L., Martinez-Cortizas, A., Mehl, I., Mesa-Fernandez, J. M., Mighall, T., Miola, A., Miras, Y., Morales-Molino, C., Mrotzek, A., Sobrino, C. Munoz, Odgaard, B., Ozola, I., Perez-Diaz, S., Perez-Obiol, R. P., Poggi, C., Rego, P. Ramil, Ramos-Roman, M. J., Rasmussen, P., Reille, M., Roesch, M., Ruffaldi, P., Goni, M. Sanchez, Savukyniene, N., Schroeder, T., Schult, M., Segerström, U., Seppae, H., Vives, G. Servera, Shumilovskikh, L., Smettan, H. W., Stancikaite, M., Stevenson, A. C., Stivrins, N., Tantau, I., Theuerkauf, M., Tonkov, S., van der Knaap, W. O., van Leeuwen, J. F. N., Vecmane, E., Verstraeten, G., Veski, S., Voigt, R., Von Stedingk, H., Waller, M. P., Wiethold, J., Willis, K. J., Wolters, S., Zernitskaya, V. P., Serge, M. A., Mazier, F., Fyfe, R., Gaillard, Marie-José, Klein, T., Lagnoux, A., Galop, D., Githumbi, Esther, Mindrescu, M., Nielsen, A. B., Trondman, Anna-Kari, Poska, A., Sugita, S., Woodbridge, J., Abel-Schaad, D., Åkesson, C., Alenius, T., Ammann, B., Andersen, S. T., Scott Anderson, R., Andric, M., Balakauskas, L., Barnekow, L., Batalova, V., Bergman, J., Birks, H. John B., Björkman, L., Bjune, A. E., Borisova, O., Broothaerts, N., Carrion, J., Caseldine, C., Christiansen, J., Cui, Q., Curras, A., Czerwinski, S., David, R., Davies, A. L., De Jong, R., Di Rita, F., Dietre, B., Doerfler, W., Doyen, E., Edwards, K. J., Ejarque, A., Endtmann, E., Etienne, D., Faure, E., Feeser, I., Feurdean, A., Fischer, E., Fletcher, W., Franco-Mugica, F., Fredh, E. D., Froyd, C., Garces-Pastor, S., Garcia-Moreiras, I., Gauthier, E., Gil-Romera, G., Gonzalez-Samperiz, P., Grant, M. J., Grindean, R., Haas, J. N., Hannon, G., Heather, A. -J, Heikkilae, M., Hjelle, K., Jahns, S., Jasiunas, N., Jimenez-Moreno, G., Jouffroy-Bapicot, I., Kabailiene, M., Kamerling, I. M., Kangur, M., Karpinska-Kolaczek, M., Kasianova, A., Kolaczek, P., Lageras, P., Latalowa, M., Lechterbeck, J., Leroyer, C., Leydet, M., Lindbladh, M., Lisitsyna, O., Lopez-Saez, J. -A, Lowe, John, Luelmo-Lautenschlaeger, R., Lukanina, E., Macijauskaite, L., Magri, D., Marguerie, D., Marquer, L., Martinez-Cortizas, A., Mehl, I., Mesa-Fernandez, J. M., Mighall, T., Miola, A., Miras, Y., Morales-Molino, C., Mrotzek, A., Sobrino, C. Munoz, Odgaard, B., Ozola, I., Perez-Diaz, S., Perez-Obiol, R. P., Poggi, C., Rego, P. Ramil, Ramos-Roman, M. J., Rasmussen, P., Reille, M., Roesch, M., Ruffaldi, P., Goni, M. Sanchez, Savukyniene, N., Schroeder, T., Schult, M., Segerström, U., Seppae, H., Vives, G. Servera, Shumilovskikh, L., Smettan, H. W., Stancikaite, M., Stevenson, A. C., Stivrins, N., Tantau, I., Theuerkauf, M., Tonkov, S., van der Knaap, W. O., van Leeuwen, J. F. N., Vecmane, E., Verstraeten, G., Veski, S., Voigt, R., Von Stedingk, H., Waller, M. P., Wiethold, J., Willis, K. J., Wolters, S., and Zernitskaya, V. P.

Abstract

Reliable quantitative vegetation reconstructions for Europe during the Holocene are crucial to improving our understanding of landscape dynamics, making it possible to assess the past effects of environmental variables and land-use change on ecosystems and biodiversity, and mitigating their effects in the future. We present here the most spatially extensive and temporally continuous pollen-based reconstructions of plant cover in Europe (at a spatial resolution of 1 degrees x 1 degrees) over the Holocene (last 11.7 ka BP) using the 'Regional Estimates of VEgetation Abundance from Large Sites' (REVEALS) model. This study has three main aims. First, to present the most accurate and reliable generation of REVEALS reconstructions across Europe so far. This has been achieved by including a larger number of pollen records compared to former analyses, in particular from the Mediterranean area. Second, to discuss methodological issues in the quantification of past land cover by using alternative datasets of relative pollen productivities (RPPs), one of the key input parameters of REVEALS, to test model sensitivity. Finally, to validate our reconstructions with the global forest change dataset. The results suggest that the RPPs.st1 (31 taxa) dataset is best suited to producing regional vegetation cover estimates for Europe. These reconstructions offer a long-term perspective providing unique possibilities to explore spatial-temporal changes in past land cover and biodiversity.

Published

2023

4. Testing the Effect of Relative Pollen Productivity on the REVEALS Model: A Validated Reconstruction of Europe-Wide Holocene Vegetation

Author

European Commission, Serge, M. A., Mazier, F., Fyfe, R., Gaillard, M. J., Klein, T., Lagnoux, A., Galop, D., Githumbi, E., Mindrescu, M., Nielsen, A. B., Trondman, A. K., Barnekow, L., Batalova, V., Bergman, J., Birks, H. John B., Björkman, L., Bjune, A. E., Borisova, O., Broothaerts, N., Carrion, J., Caseldine, C., Grindean, R., Christiansen, J., Cui, Q., Currás, Andrés, Czerwiński, S., David, R., Davies, A. L., De Jong, R., Di Rita, F., Dietre, B., Dörfler, W., Haas, J. N., Doyen, E., Edwards, K. J., Ejarque, A., Endtmann, E., Etienne, D., Faure, E., Feeser, I., Feurdean, A., Fischer, E., Fletcher, W., Hannon, G., Franco-Múgica, F., Fredh, E. D., Froyd, C., Garcés-Pastor, S., García-Moreiras, I., Gauthier, E., Gil-Romera, Graciela, González-Sampériz, Penélope, Grant, M. J., Heather, A. J., Heikkilä, M., Hjelle, K., Jahns, S., Jasiunas, N., Jiménez-Moreno, G., Jouffroy-Bapicot, I., Sobrino, C. Muñoz, Kabailienė, M., Kamerling, I. M., Kangur, M., Karpińska-Kołaczek, M., Kasianova, A., Kołaczek, P., Lagerås, P., Latalowa, M., Lechterbeck, J., Leroyer, C., Odgaard, B., Leydet, M., Lindbladh, M., Lisitsyna, O., López Sáez, José Antonio, Lowe, John, Luelmo Lautenschlaeger, Reyes, Lukanina, E., Macijauskaitė, L., Magri, D., Marguerie, D., Ozola, I., Marquer, L., Martínez Cortizas, Antonio, Mehl, I., Mesa-Fernández, J. M., Mighall, Tim, Miola, A., Miras, Y., Morales-Molino, C., Mrotzek, A., Pérez-Díaz, S., Pérez-Obiol, R. P., Poggi, C., Rego, P. Ramil, Ramos-Román, M. J., Rasmussen, P., Reille, M., Poska, A., Rösch, M., Ruffaldi, P., Goni, M. Sánchez, Savukynienė, N., Schröder, T., Schult, M., Segerström, U., Seppä, H., Vives, G. Servera, Shumilovskikh, L., Sugita, S., Smettan, H. W., Stancikaite, M., Stevenson, A. C., Stivrins, N., Tantau, I., Theuerkauf, M., Tonkov, S., van der Knaap, W. O., van Leeuwen, J. F. N., Vecmane, E., Woodbridge, J., Verstraeten, G., Veski, S., Voigt, R., Von Stedingk, H., Waller, M. P., Wiethold, J., Willis, K. J., Wolters, S., Zernitskaya, V. P., Abel-Schaad, D., Åkesson, C., Alenius, T., Ammann, B., Andersen, S. T., Anderson, R. Scott, Andrič, M., Balakauskas, L., European Commission, Serge, M. A., Mazier, F., Fyfe, R., Gaillard, M. J., Klein, T., Lagnoux, A., Galop, D., Githumbi, E., Mindrescu, M., Nielsen, A. B., Trondman, A. K., Barnekow, L., Batalova, V., Bergman, J., Birks, H. John B., Björkman, L., Bjune, A. E., Borisova, O., Broothaerts, N., Carrion, J., Caseldine, C., Grindean, R., Christiansen, J., Cui, Q., Currás, Andrés, Czerwiński, S., David, R., Davies, A. L., De Jong, R., Di Rita, F., Dietre, B., Dörfler, W., Haas, J. N., Doyen, E., Edwards, K. J., Ejarque, A., Endtmann, E., Etienne, D., Faure, E., Feeser, I., Feurdean, A., Fischer, E., Fletcher, W., Hannon, G., Franco-Múgica, F., Fredh, E. D., Froyd, C., Garcés-Pastor, S., García-Moreiras, I., Gauthier, E., Gil-Romera, Graciela, González-Sampériz, Penélope, Grant, M. J., Heather, A. J., Heikkilä, M., Hjelle, K., Jahns, S., Jasiunas, N., Jiménez-Moreno, G., Jouffroy-Bapicot, I., Sobrino, C. Muñoz, Kabailienė, M., Kamerling, I. M., Kangur, M., Karpińska-Kołaczek, M., Kasianova, A., Kołaczek, P., Lagerås, P., Latalowa, M., Lechterbeck, J., Leroyer, C., Odgaard, B., Leydet, M., Lindbladh, M., Lisitsyna, O., López Sáez, José Antonio, Lowe, John, Luelmo Lautenschlaeger, Reyes, Lukanina, E., Macijauskaitė, L., Magri, D., Marguerie, D., Ozola, I., Marquer, L., Martínez Cortizas, Antonio, Mehl, I., Mesa-Fernández, J. M., Mighall, Tim, Miola, A., Miras, Y., Morales-Molino, C., Mrotzek, A., Pérez-Díaz, S., Pérez-Obiol, R. P., Poggi, C., Rego, P. Ramil, Ramos-Román, M. J., Rasmussen, P., Reille, M., Poska, A., Rösch, M., Ruffaldi, P., Goni, M. Sánchez, Savukynienė, N., Schröder, T., Schult, M., Segerström, U., Seppä, H., Vives, G. Servera, Shumilovskikh, L., Sugita, S., Smettan, H. W., Stancikaite, M., Stevenson, A. C., Stivrins, N., Tantau, I., Theuerkauf, M., Tonkov, S., van der Knaap, W. O., van Leeuwen, J. F. N., Vecmane, E., Woodbridge, J., Verstraeten, G., Veski, S., Voigt, R., Von Stedingk, H., Waller, M. P., Wiethold, J., Willis, K. J., Wolters, S., Zernitskaya, V. P., Abel-Schaad, D., Åkesson, C., Alenius, T., Ammann, B., Andersen, S. T., Anderson, R. Scott, Andrič, M., and Balakauskas, L.

Abstract

Reliable quantitative vegetation reconstructions for Europe during the Holocene are crucial to improving our understanding of landscape dynamics, making it possible to assess the past effects of environmental variables and land-use change on ecosystems and biodiversity, and mitigating their effects in the future. We present here the most spatially extensive and temporally continuous pollen-based reconstructions of plant cover in Europe (at a spatial resolution of 1° × 1°) over the Holocene (last 11.7 ka BP) using the ‘Regional Estimates of VEgetation Abundance from Large Sites’ (REVEALS) model. This study has three main aims. First, to present the most accurate and reliable generation of REVEALS reconstructions across Europe so far. This has been achieved by including a larger number of pollen records compared to former analyses, in particular from the Mediterranean area. Second, to discuss methodological issues in the quantification of past land cover by using alternative datasets of relative pollen productivities (RPPs), one of the key input parameters of REVEALS, to test model sensitivity. Finally, to validate our reconstructions with the global forest change dataset. The results suggest that the RPPs.st1 (31 taxa) dataset is best suited to producing regional vegetation cover estimates for Europe. These reconstructions offer a long-term perspective providing unique possibilities to explore spatial-temporal changes in past land cover and biodiversity.

Published

2023

5. Chapter 4. Biomarkers of Exposure: Hemoglobin Adducts

Author

von Stedingk, H., primary, Osterman-Golkar, S., additional, and Törnqvist, M., additional

Published

2011

6. Enhanced susceptibility of obese mice to glycidamide-induced sperm chromatin damage without increased oxidative stress

Author

Gutzkow, K. B., primary, Duale, N., additional, Danielsen, T., additional, von Stedingk, H., additional, Shahzadi, S., additional, Instanes, C., additional, Olsen, A.-K., additional, Steffensen, I.-L., additional, Hofer, T., additional, Törnqvist, M., additional, Brunborg, G., additional, and Lindeman, B., additional

Published

2016

7. Birth weight, head circumference, and prenatal exposure to acrylamide from maternal diet: The European prospective mother-child study (NewGeneris)

Author

Pedersen, M, von Stedingk, H, Botsivali, M, Agramunt, S, Alexander, J, Brunborg, G, Chatzi, L, Fleming, S, Fthenou, E, Granum, B, Gutzkow, KB, Hardie, LJ, Knudsen, LE, Kyrtopoulos, SA, Mendez, MA, Merlo, DF, Nielsen, JK, Rydberg, P, Segerbäck, D, Sunyer, J, Wright, J, Törnqvist, M, Kleinjans, JC, Kogevinas, M, Burley, VJ, Carreras, R, Fontana, V, de Kok, TM, Haugen, M, Hemminki, K, Kirsch-Volders, M, Koutis, A, Løvik, M, McKinney, PA, Meltzer, HM, Mijal, R, Stagi, E, van Brenda, SGJ, Wild, CP, Toxicogenomics, and RS: GROW - School for Oncology and Reproduction

Subjects

Health, Toxicology and Mutagenesis, Embaràs, Developmental toxicity, Physiology, Intrauterine growth restriction, Biochemistry, Mass Spectrometry, Cohort Studies, chemistry.chemical_compound, Hemoglobins, Pregnancy, Surveys and Questionnaires, Birth Weight, Prospective Studies, Children, News | Science Selections, Diet and Nutrition, Acrylamide, Chemistry, Environmental exposure, Fetal Blood, Infants -- Alimentació, Europe, Reproductive Health, Maternal Exposure, Anatomy & histology, Prenatal Exposure Delayed Effects, Children's Health, Regression Analysis, Environmental Pollutants, Female, medicine.symptom, Environmental Monitoring, Adult, medicine.medical_specialty, Birth weight, Disruptors endocrins, In utero exposure, medicine, Humans, International Environmental Health, Research, Public Health, Environmental and Occupational Health, Infant, Newborn, Environmental Exposure, Biomarker, Infant, Low Birth Weight, medicine.disease, Surgery, Diet, Low birth weight, Epoxy Compounds, Head, Chromatography, Liquid

Abstract

Background: Acrylamide is a common dietary exposure that crosses the human placenta. It is classified as a probable human carcinogen, and developmental toxicity has been observed in rodents. Objectives: We examined the associations between prenatal exposure to acrylamide and birth outcomes in a prospective European mother–child study. Methods: Hemoglobin (Hb) adducts of acrylamide and its metabolite glycidamide were measured in cord blood (reflecting cumulated exposure in the last months of pregnancy) from 1,101 singleton pregnant women recruited in Denmark, England, Greece, Norway, and Spain during 2006–2010. Maternal diet was estimated through food-frequency questionnaires. Results: Both acrylamide and glycidamide Hb adducts were associated with a statistically significant reduction in birth weight and head circumference. The estimated difference in birth weight for infants in the highest versus lowest quartile of acrylamide Hb adduct levels after adjusting for gestational age and country was –132 g (95% CI: –207, –56); the corresponding difference for head circumference was –0.33 cm (95% CI: –0.61, –0.06). Findings were similar in infants of nonsmokers, were consistent across countries, and remained after adjustment for factors associated with reduced birth weight. Maternal consumption of foods rich in acrylamide, such as fried potatoes, was associated with cord blood acrylamide adduct levels and with reduced birth weight. Conclusions: Dietary exposure to acrylamide was associated with reduced birth weight and head circumference. Consumption of specific foods during pregnancy was associated with higher acrylamide exposure in utero. If confirmed, these findings suggest that dietary intake of acrylamide should be reduced among pregnant women. The NewGeneris (Newborns and Genotoxic exposure risks) study was funded by the European Union (EU Contract FOOD-CT-2005-016320). The study was also supported by grants obtained locally, including the Swedish Cancer and Allergy Foundation and the Swedish Research Council Formas, the National Institute for Health Research, UK (programme grant RP-PG-0407-10044), the Norwegian Ministry of Health, the Norwegian Ministry of Education and Research, the Norwegian Research Council/FUGE (grant 151918/S10), the EU funded HiWATE (contract Food-CT-2006-036224), the U.S. National Institutes of Health (NIH)/National Institute of Environmental Health Sciences (contract NO-ES-75558), and the U.S. NIH/National Institute of Neurological Disorders and Stroke (grant 1 UO1 NS 047537-01). M.P. holds a Juan de la Cierva postdoctoral fellowship awarded from the Spanish Ministry of Science and Innovation (JCI-2011-09479)

Published

2012

8. DNA from soil mirrors plant taxonomic and growth form diversity

Author

Yoccoz, N.G., Bråthen, K.A., Gielly, L., Haile, J., Edwards, M.E., Goslar, T., Von Stedingk, H., Brysting, A.K., Coissac, E., Pompanan, F., Sonstebo, J.H., Miquel, C., Valentini, A., De Bello, F., Chave, J, Thuiller, W., Wincker, P., Cruaud, C., Gavory, F., Rasmussen, M., Gilbert, M.T.P., Orlando, L., Brochmann, C., Willerslev, E., Taberlet, P., Yoccoz, N.G., Bråthen, K.A., Gielly, L., Haile, J., Edwards, M.E., Goslar, T., Von Stedingk, H., Brysting, A.K., Coissac, E., Pompanan, F., Sonstebo, J.H., Miquel, C., Valentini, A., De Bello, F., Chave, J, Thuiller, W., Wincker, P., Cruaud, C., Gavory, F., Rasmussen, M., Gilbert, M.T.P., Orlando, L., Brochmann, C., Willerslev, E., and Taberlet, P.

Abstract

Ecosystems across the globe are threatened by climate change and human activities. New rapid survey approaches for monitoring biodiversity would greatly advance assessment and understanding of these threats. Taking advantage of next-generation DNA sequencing, we tested an approach we call metabarcoding: high-throughput and simultaneous taxa identification based on a very short (usually <100 base pairs) but informative DNA fragment. Short DNA fragments allow the use of degraded DNA from environmental samples. All analyses included amplification using plant-specific versatile primers, sequencing and estimation of taxonomic diversity. We tested in three steps whether degraded DNA from dead material in soil has the potential of efficiently assessing biodiversity in different biomes. First, soil DNA from eight boreal plant communities located in two different vegetation types (meadow and heath) was amplified. Plant diversity detected from boreal soil was highly consistent with plant taxonomic and growth form diversity estimated from conventional above-ground surveys. Second, we assessed DNA persistence using samples from formerly cultivated soils in temperate environments. We found that the number of crop DNA sequences retrieved strongly varied with years since last cultivation, and crop sequences were absent from nearby, uncultivated plots. Third, we assessed the universal applicability of DNA metabarcoding using soil samples from tropical environments: a large proportion of species and families from the study site were efficiently recovered. The results open unprecedented opportunities for large-scale DNA-based biodiversity studies across a range of taxonomic groups using standardized metabarcoding approaches.

Published

2012

9. DNA from soil mirrors plant taxonomic and growth form diversity

Author

Yoccoz, N. G., Bråthen, K. A., Gielly, L., Haile, James Seymour, Edwards, M. E., Goslar, T., von Stedingk, H., Brysting, A. K., Coissac, E., Pompanon, F., Sønstebo, J. H., Miquel, C., Valentini, A., de Bello, F., Chave, J., Thuiller, W., Wincker, P., Cruaud, C., Gavory, F., Rasmussen, Morten, Gilbert, Tom, Orlando, Ludovic Antoine Alexandre, Brochmann, C., Willerslev, Eske, Taberlet, P., Yoccoz, N. G., Bråthen, K. A., Gielly, L., Haile, James Seymour, Edwards, M. E., Goslar, T., von Stedingk, H., Brysting, A. K., Coissac, E., Pompanon, F., Sønstebo, J. H., Miquel, C., Valentini, A., de Bello, F., Chave, J., Thuiller, W., Wincker, P., Cruaud, C., Gavory, F., Rasmussen, Morten, Gilbert, Tom, Orlando, Ludovic Antoine Alexandre, Brochmann, C., Willerslev, Eske, and Taberlet, P.

Abstract

Ecosystems across the globe are threatened by climate change and human activities. New rapid survey approaches for monitoring biodiversity would greatly advance assessment and understanding of these threats. Taking advantage of next-generation DNA sequencing, we tested an approach we call metabarcoding: high-throughput and simultaneous taxa identification based on a very short (usually

Published

2012

10. DNA from soil mirrors plant taxonomic and growth form diversity

Author

Yoccoz, N., Brathen, K., Gielly, L., Haile, James, Edwards, M., Goslar, T., Von Stedingk, H., Brysting, A., Coissac, E., Pompanon, F., Sonstebo, J., Miquel, C., Valentini, A., De Bello, F., Chave, J., Thuiller, W., Wincker, P., Cruaud, C., Gavory, F., Rasmussen, M., Gilbert, Thomas, Orlando, L., Brochmann, C., Willerslev, E., Taberlet, P., Yoccoz, N., Brathen, K., Gielly, L., Haile, James, Edwards, M., Goslar, T., Von Stedingk, H., Brysting, A., Coissac, E., Pompanon, F., Sonstebo, J., Miquel, C., Valentini, A., De Bello, F., Chave, J., Thuiller, W., Wincker, P., Cruaud, C., Gavory, F., Rasmussen, M., Gilbert, Thomas, Orlando, L., Brochmann, C., Willerslev, E., and Taberlet, P.

Abstract

Ecosystems across the globe are threatened by climate change and human activities. New rapid survey approaches for monitoring biodiversity would greatly advance assessment and understanding of these threats. Taking advantage of next-generation DNA sequencing, we tested an approach we call metabarcoding: high-throughput and simultaneous taxa identification based on a very short (usually <100 base pairs) but informative DNA fragment. Short DNA fragments allow the use of degraded DNA from environmental samples. All analyses included amplification using plant-specific versatile primers, sequencing and estimation of taxonomic diversity. We tested in three steps whether degraded DNA from dead material in soil has the potential of efficiently assessing biodiversity in different biomes. First, soil DNA from eight boreal plant communities located in two different vegetation types (meadow and heath) was amplified. Plant diversity detected from boreal soil was highly consistent with planttaxonomic and growth form diversity estimated from conventional above-ground surveys. Second, we assessed DNA persistence using samples from formerly cultivated soils in temperate environments. We found that the number of crop DNA sequences retrieved strongly varied with years since last cultivation, and crop sequences were absent from nearby, uncultivated plots. Third, we assessed the universal applicability of DNA metabarcoding using soil samples from tropical environments: a large proportion of species and families from the study site were efficiently recovered. The results openunprecedented opportunities for large-scale DNA-based biodiversity studies across a range of taxonomic groups using standardized metabarcoding approaches.

Published

2012

11. Holocene land-cover reconstructions for studies on land cover-climate feedbacks

Author

Gaillard, Marie-José, Sugita, Shinya, Mazier, Florence, Trondman, Anna-Kari, Broström, A, Hickler, T, Kaplan, J.O., Kjellström, E, Kokfelt, U, Kunes, P, Lemmen, C, Miller, P, Olofsson, J, Poska, A, Rundgren, M, Smith, B, Strandberg, G, Fyfe, R, Nielsen, A.B., Alenius, T, Balakauskas, L, Barnekov, L, Birks, H.J.B., Bjune, A, Bjorkman, L, Giesecke, T, Hjelle, K, Kalnina, L, Kangur, M, van der Knaap, W.O., Koff, T, Lageras, P, Latalowa, M, Leydet, M, Lechterbeck, J, Lindbladh, M, Odgaard, B, Peglar, S, Segerstrom, U, von Stedingk, H, Seppa, H, Gaillard, Marie-José, Sugita, Shinya, Mazier, Florence, Trondman, Anna-Kari, Broström, A, Hickler, T, Kaplan, J.O., Kjellström, E, Kokfelt, U, Kunes, P, Lemmen, C, Miller, P, Olofsson, J, Poska, A, Rundgren, M, Smith, B, Strandberg, G, Fyfe, R, Nielsen, A.B., Alenius, T, Balakauskas, L, Barnekov, L, Birks, H.J.B., Bjune, A, Bjorkman, L, Giesecke, T, Hjelle, K, Kalnina, L, Kangur, M, van der Knaap, W.O., Koff, T, Lageras, P, Latalowa, M, Leydet, M, Lechterbeck, J, Lindbladh, M, Odgaard, B, Peglar, S, Segerstrom, U, von Stedingk, H, and Seppa, H

Abstract

The major objectives of this paper are: (1) to review the pros and cons of the scenarios of past anthropogenic land cover change (ALCC) developed during the last ten years, (2) to discuss issues related to pollen-based reconstruction of the past land-cover and introduce a new method, REVEALS (Regional Estimates of VEgetation Abundance from Large Sites), to infer long-term records of past land-cover from pollen data, (3) to present a new project (LANDCLIM: LAND cover – CLIMate interactions in NW Europe during the Holocene) currently underway, and show preliminary results of REVEALS reconstructions of the regional land-cover in the Czech Republic for five selected time windows of the Holocene, and (4) to discuss the implications and future directions in climate and vegetation/land-cover modeling, and in the assessment of the effects of human-induced changes in land-cover on the regional climate through altered feedbacks. The existing ALCC scenarios show large discrepancies between them, and few cover time periods older than AD 800. When these scenarios are used to assess the impact of human land-use on climate, contrasting results are obtained. It emphasizes the need for methods such as the REVEALS model-based land-cover reconstructions. They might help to fine-tune descriptions of past land-cover and lead to a better understanding of how long-term changes in ALCC might have influenced climate. The REVEALS model is demonstrated to provide better estimates of the regional vegetation/landcover changes than the traditional use of pollen percentages. This will achieve a robust assessment of land cover at regional- to continental-spatial scale throughout the Holocene. We present maps of REVEALS estimates for the percentage cover of 10 plant functional types (PFTs) at 200 BP and 6000 BP, and of the two open-land PFTs “grassland” and “agricultural land” at five time-windows from 6000 BP to recent time. The LANDCLIM results are expected to provide crucial data to reassess ALC, NordForsk LANDCLIM, VR LANDCLIM, MERGE

Published

2010

12. DNA from soil mirrors plant taxonomic and growth form diversity

Author

YOCCOZ, N. G., primary, BRÅTHEN, K. A., additional, GIELLY, L., additional, HAILE, J., additional, EDWARDS, M. E., additional, GOSLAR, T., additional, Von STEDINGK, H., additional, BRYSTING, A. K., additional, COISSAC, E., additional, POMPANON, F., additional, SØNSTEBØ, J. H., additional, MIQUEL, C., additional, VALENTINI, A., additional, De BELLO, F., additional, CHAVE, J., additional, THUILLER, W., additional, WINCKER, P., additional, CRUAUD, C., additional, GAVORY, F., additional, RASMUSSEN, M., additional, GILBERT, M. T. P., additional, ORLANDO, L., additional, BROCHMANN, C., additional, WILLERSLEV, E., additional, and TABERLET, P., additional

Published

2012

13. Holocene land-cover reconstructions for studies on land cover-climate feedbacks

Author

Gaillard, M.-J., primary, Sugita, S., additional, Mazier, F., additional, Trondman, A.-K., additional, Broström, A., additional, Hickler, T., additional, Kaplan, J. O., additional, Kjellström, E., additional, Kokfelt, U., additional, Kuneš, P., additional, Lemmen, C., additional, Miller, P., additional, Olofsson, J., additional, Poska, A., additional, Rundgren, M., additional, Smith, B., additional, Strandberg, G., additional, Fyfe, R., additional, Nielsen, A. B., additional, Alenius, T., additional, Balakauskas, L., additional, Barnekow, L., additional, Birks, H. J. B., additional, Bjune, A., additional, Björkman, L., additional, Giesecke, T., additional, Hjelle, K., additional, Kalnina, L., additional, Kangur, M., additional, van der Knaap, W. O., additional, Koff, T., additional, Lagerås, P., additional, Latałowa, M., additional, Leydet, M., additional, Lechterbeck, J., additional, Lindbladh, M., additional, Odgaard, B., additional, Peglar, S., additional, Segerström, U., additional, von Stedingk, H., additional, and Seppä, H., additional

Published

2010

14. Holocene biomass burning and gloibal dynamics of carbon cycle

Author

Carcaillet, C, Almquist, H, Asnong, H, Bradshaw, R H W, Carrion, J S, Gaillard, Marie-Jose, Gajewski, K, Haas, J N, Haberle, S G, Hadorn, P, Müller, S D, Richard, P J H, Richoz, I, Rösch, M, Sanchez Goni, M F, von Stedingk, H, Stevenson, A C, Talon, B, Tardy, C, Tinner, W, Tryterud, E, Wick, L, Willis, K J, Carcaillet, C, Almquist, H, Asnong, H, Bradshaw, R H W, Carrion, J S, Gaillard, Marie-Jose, Gajewski, K, Haas, J N, Haberle, S G, Hadorn, P, Müller, S D, Richard, P J H, Richoz, I, Rösch, M, Sanchez Goni, M F, von Stedingk, H, Stevenson, A C, Talon, B, Tardy, C, Tinner, W, Tryterud, E, Wick, L, and Willis, K J

Published

2002

15. Holocene biomass burning and global dynamics of the carbon cycle

Author

Carcaillet, C., primary, Almquist, H., additional, Asnong, H., additional, Bradshaw, R.H.W., additional, Carrión, J.S., additional, Gaillard, M.-J., additional, Gajewski, K., additional, Haas, J.N., additional, Haberle, S.G., additional, Hadorn, P., additional, Müller, S.D., additional, Richard, P.J.H., additional, Richoz, I., additional, Rösch, M., additional, Sánchez Goñi, M.F., additional, von Stedingk, H., additional, Stevenson, A.C., additional, Talon, B., additional, Tardy, C., additional, Tinner, W., additional, Tryterud, E., additional, Wick, L., additional, and Willis, K.J., additional

Published

2002

16. Ethylene Oxide Hemoglobin Adducts in Cord Blood and Offspring's Size at Birth: The NewGeneris European Cohort Study.

Author

Harding BN, Agramunt S, Pedersen M, Knudsen LE, Nielsen JKS, Wright J, Vafeiadi M, Merlo DF, Stayner L, Kelly-Reif K, Espinosa A, Bustamante M, Gützkow KB, Granum B, von Stedingk H, Rydberg P, Alexander J, Törnqvist M, and Kogevinas M

Subjects

Humans, Female, Infant, Newborn, Pregnancy, Prospective Studies, Male, Europe, Adult, Polymorphism, Single Nucleotide, Maternal Exposure adverse effects, Prenatal Exposure Delayed Effects, Linear Models, Infant, Small for Gestational Age, Cohort Studies, Fetal Blood chemistry, Birth Weight drug effects, Cytochrome P-450 CYP2E1 genetics, Hemoglobins analysis, Ethylene Oxide

Abstract

Background: Prenatal ethylene oxide exposure may have adverse effects on fetal development. We examined the relationships between ethylene oxide hemoglobin (Hb) adduct levels and offspring's size at birth in a prospective European mother-child study., Methods: This study included 1106 singletons from the NewGeneris project (2006-2010) with ethylene oxide Hb adducts measured in cord blood. We examined the relationships between adduct levels and offspring's size at birth among all infants and separately among infants of nonsmokers, using linear regression models for birth weight and birth head circumference and logarithmic binomial regression models for small for gestational age. We examined potential interactions between CYP2E1 single nucleotide polymorphisms in cord blood and the effects of ethylene oxide Hb adduct levels on offspring birth size., Results: Higher quartiles of adduct levels as a measure of exposure were associated with decreasing birth weight and head circumference in the overall population. Compared to infants in the lowest quartile, those in the highest quartile exhibited lower birth weight (-70.73 g, 95% confidence interval = -141.16, -0.30) and reduced head circumference (-0.30 cm, 95% confidence interval = -0.58, -0.02). We observed similar, albeit less pronounced, patterns among infants of nonsmokers. There was no evidence of an association between ethylene oxide Hb adducts and risk of small for gestational age, nor consistent evidence of an interaction with CYP2E1 polymorphisms on the association between EO Hb adduct levels and offspring's size at birth., Conclusion: Results suggest that higher ethylene oxide Hb adduct levels in cord blood are associated with a reduction in offspring birth size., Competing Interests: Disclosure: The authors report no conflicts of interest., (Copyright © 2024 The Author(s). Published by Wolters Kluwer Health, Inc.)

Published

2024

17. What does FSC forest certification contribute to biodiversity conservation in relation to national legislation?

Author

Lehtonen E, Gustafsson L, Lõhmus A, and von Stedingk H

Subjects

Biodiversity, Certification, Forests, Conservation of Natural Resources, Forestry

Abstract

Forest certification has emerged as a voluntary, market-driven tool for sustainable forest management (SFM). Its legitimacy depends on its ability to achieve its objectives and to retain the support of stakeholders such as NGOs and the companies that adopt it. This study presents a novel approach for assessing the contributions of forest certification to biodiversity conservation, based on Forest Stewardship Council (FSC) certification in four northern European countries (Finland, Sweden, Estonia, Latvia). In each case, national FSC certification requirements related to specific biodiversity targets were compared with requirements in national legislation. Nearly 80% of the assessed certification requirements were more prescriptive than the national legislation. One-third of these requirements (3-8 per country) were assessed to have a positive contribution to biodiversity conservation, whereas four requirements (up to 2 per country) were assessed to have a low positive contribution. FSC requirements to protect Woodland Key Habitats were identified as having a positive contribution in all four countries, whereas requirements regarding live tree retention in harvests and preserving dead wood had a positive contribution in three countries each. Despite often prescribing similar measures, the other requirements with positive contributions varied between countries depending on the national legislative baseline. The remaining requirements could not be assessed through expert evaluation, indicating the need for additional empirical research to evaluate how the normative requirements translate to impacts in the field, and how the national context may affect their implementation. The approach is globally applicable, repeatable, and provides a basis for designing systematic empirical assessments of the certification impact., (Copyright © 2021 Elsevier Ltd. All rights reserved.)

Published

2021

18. Maternal diet during pregnancy and micronuclei frequency in peripheral blood T lymphocytes in mothers and newborns (Rhea cohort, Crete).

Author

O'Callaghan-Gordo C, Kogevinas M, Pedersen M, Fthenou E, Espinosa A, Tsiapa X, Chalkiadaki G, Daraki V, Dermitzaki E, Decordier I, Farmer PB, Georgiadis P, Georgiou V, Kyrtopoulos SA, Merlo DF, Romaguera D, Roumeliotaki T, Sarri K, Törnqvist M, Loock KV, von Stedingk H, Kleinjans J, Kirsch-Volders M, and Chatzi L

Subjects

Adult, Biomarkers, Tumor genetics, Carcinogens administration & dosage, Environmental Exposure, Female, Fetal Blood cytology, Greece, Humans, Infant, Newborn, Male, Maternal Exposure, Maternal-Fetal Exchange, Mothers, Neoplasms prevention & control, Pregnancy, Prenatal Exposure Delayed Effects, Red Meat adverse effects, Diet, Micronuclei, Chromosome-Defective statistics & numerical data, Neoplasms genetics, T-Lymphocytes ultrastructure

Abstract

Purpose: The study assessed whether diet and adherence to cancer prevention guidelines during pregnancy were associated with micronucleus (MN) frequency in mothers and newborns. MN is biomarkers of early genetic effects that have been associated with cancer risk in adults., Methods: A total of 188 mothers and 200 newborns from the Rhea cohort (Greece) were included in the study. At early-mid pregnancy, we conducted personal interviews and a validated food frequency questionnaire was completed. With this information, we constructed a score reflecting adherence to the World Cancer Research Fund/American Institute for Cancer Research cancer prevention guidelines on diet, physical activity and body fatness. At delivery, maternal and/or cord blood was collected to measure DNA and hemoglobin adducts of dietary origin and frequencies of MN in binucleated and mononucleated T lymphocytes (MNBN and MNMONO)., Results: In mothers, higher levels of red meat consumption were associated with increased MNBN frequency [2nd tertile IRR = 1.34 (1.00, 1.80), 3rd tertile IRR = 1.33 (0.96, 1.85)] and MNMONO frequency [2nd tertile IRR = 1.53 (0.84, 2.77), 3rd tertile IRR = 2.69 (1.44, 5.05)]. The opposite trend was observed for MNBN in newborns [2nd tertile IRR = 0.64 (0.44, 0.94), 3rd tertile IRR = 0.68 (0.46, 1.01)], and no association was observed with MNMONO. Increased MN frequency in pregnant women with high red meat consumption is consistent with previous knowledge., Conclusions: Our results also suggest exposure to genotoxics during pregnancy might affect differently mothers and newborns. The predictive value of MN as biomarker for childhood cancer, rather than adulthood, remains unclear. With few exceptions, the association between maternal carcinogenic exposures during pregnancy and childhood cancer or early biologic effect biomarkers remains poorly understood.

Published

2018

19. Effects of benthos, temperature, and dose on the fate of hexabromocyclododecane in experimental coastal ecosystems.

Author

Bradshaw C, Strid A, von Stedingk H, and Gustafsson K

Subjects

Animals, Bivalvia, Ecosystem, Geologic Sediments analysis, Hydrocarbons, Brominated analysis, Phytoplankton chemistry, Phytoplankton metabolism, Stereoisomerism, Flame Retardants analysis, Hydrocarbons, Brominated chemistry, Temperature, Water Pollutants, Chemical chemistry

Abstract

The authors studied the fate of the brominated flame retardant hexabromocyclododecane (HBCDD) added in a particulate suspension to experimental ecosystems assembled from brackish (Baltic Sea) coastal bays. Two experiments examined how benthic macrofauna (over 21 d) and increased temperature (14 d) affected HBCDD concentrations and fractionation of α, β, and γ diastereomers in the water, sediment, and biota. A third experiment run over 3 seasons (231 d), studied the effect of HBCDD dose on the same endpoints. In all treatments of the 3 experiments, HBCDD partitioned mainly to the sediment, and this proportion increased with time. Presence of macrofauna tended to increase the HBCDD concentration in the sediment and decreased its concentration in the water. Increased temperature (+ 5°C) decreased the amount of HBCDD in sediment and water but not in the filter- and deposit-feeding infaunal bivalves (Macoma balthica). The partitioning between water, sediment, and biota was not concentration dependent. In all treatments, sediment became enriched in γ-HBCDD, M. balthica in α-HBCDD, and water in α- and β-HBCDD. Bioaccumulation of HBCDD in M. balthica was high in all experiments (log biota-sediment accumulation factor [BSAF] > 1.25), the α diastereomer contributing the most (log BSAF 2.1-5.2). There is a risk of trophic transfer of HBCDD from benthic to pelagic food webs, as well as secondary poisoning of marine consumers., (© 2015 SETAC.)

Published

2015

20. LC-MS/MS screening strategy for unknown adducts to N-terminal valine in hemoglobin applied to smokers and nonsmokers.

Author

Carlsson H, von Stedingk H, Nilsson U, and Törnqvist M

Subjects

Case-Control Studies, Humans, Chromatography, Liquid methods, Hemoglobins chemistry, Smoking blood, Tandem Mass Spectrometry methods, Valine analysis

Abstract

Electrophilically reactive compounds have the ability to form adducts with nucleophilic sites in DNA and proteins, constituting a risk for toxic effects. Mass spectrometric detection of adducts to N-terminal valine in hemoglobin (Hb) after detachment by modified Edman degradation procedures is one approach for in vivo monitoring of exposure to electrophilic compounds/metabolites. So far, applications have been limited to one or a few selected reactive species, such as acrylamide and its metabolite glycidamide. This article presents a novel screening strategy for unknown Hb adducts to be used as a basis for an adductomic approach. The method is based on a modified Edman procedure, FIRE, specifically developed for LC-MS/MS analysis of N-terminal valine adducts in Hb detached as fluorescein thiohydantoin (FTH) derivatives. The aim is to detect and identify a priori unknown Hb adducts in human blood samples. Screening of valine adducts was performed by stepwise scanning of precursor ions in small mass increments, monitoring four fragments common for the FTH derivative of valine with different N-substitutions in the multiple-reaction mode, covering a mass range of 135 Da (m/z 503-638). Samples from six smokers and six nonsmokers were analyzed. Control experiments were performed to compare these results with known adducts and to check for artifactual formation of adducts. In all samples of smokers and nonsmokers, seven adducts were identified, of which six have previously been studied. Nineteen unknown adducts were observed, and 14 of those exhibited fragmentation patterns similar to earlier studied FTH derivatives of adducts to valine. Identification of the unknown adducts will be the focus of future work. The presented methodology is a promising screening tool using Hb adducts to indicate exposure to potentially toxic electrophilic compounds and metabolites.

Published

2014

21. Validation of a novel procedure for quantification of the formation of phosphoramide mustard by individuals treated with cyclophosphamide.

Author

von Stedingk H, Xie H, Hatschek T, Foukakis T, Rydén A, Bergh J, and Rydberg P

Subjects

Antineoplastic Combined Chemotherapy Protocols pharmacology, Antineoplastic Combined Chemotherapy Protocols therapeutic use, Biomarkers, Biomarkers, Pharmacological blood, Breast Neoplasms drug therapy, Calibration, Female, Hemoglobins chemistry, Hemoglobins metabolism, Humans, Limit of Detection, Tandem Mass Spectrometry methods, Blood Chemical Analysis methods, Cyclophosphamide pharmacology, Phosphoramide Mustards blood

Abstract

Purpose: Use of the patient's body surface area (mg m(-2)) as a basis for dosing does not take individual variation in metabolic capacity and rate of clearance into account. Here, we evaluated a novel approach for individual monitoring of short-lived cytotoxic agents formed from cytostatic drugs such as cyclophosphamide (CP)., Methods: The accumulated blood dose of the cytotoxic active agent phosphoramide mustard (PAM) formed from CP was measured as a reaction product with hemoglobin (Hb adduct). This adduct, N-[2-(2-oxazolidonyl)ethyl]-valyl Hb (OzVal-Hb), was detached from Hb with the adduct FIRE procedure™, and the formed analyte was quantified using LC-MS/MS. This dose biomarker for PAM and the analytical procedure was evaluated in accordance with the guidelines on bioanalytical method validation formulated by the European Medicine Agency. The evaluated method was applied to quantify blood dose levels of PAM in female breast cancer patients (n = 12) before and after three cycles of polychemotherapy regimes containing CP., Results: OzVal-Hb, a specific and stable biomarker, could be measured with great sensitivity (lower limit of quantification = 33 pmol g(-1) Hb), high accuracy (within ±20 %) and good repeatability (CV < 20 %). The inter-individual variability in the blood level of this adduct in women with breast cancer (n = 12) who received three doses of CP in combination with one or two other cytostatic drugs was 250 % following the first dose and approximately 150 % after each subsequent dose., Conclusions: Measurement of the biomarker OzVal-Hb can be used to quantify the short-lived cytotoxic agent PAM in a single blood sample drawn several days after therapy. This procedure may aid in individualizing doses of CP, thereby improving efficacy while both reducing the risk of and increasing the predictability of side-effects.

Published

2014

22. Micronuclei in cord blood lymphocytes and associations with biomarkers of exposure to carcinogens and hormonally active factors, gene polymorphisms, and gene expression: the NewGeneris cohort.

Author

Merlo DF, Agramunt S, Anna L, Besselink H, Botsivali M, Brady NJ, Ceppi M, Chatzi L, Chen B, Decordier I, Farmer PB, Fleming S, Fontana V, Försti A, Fthenou E, Gallo F, Georgiadis P, Gmuender H, Godschalk RW, Granum B, Hardie LJ, Hemminki K, Hochstenbach K, Knudsen LE, Kogevinas M, Kovács K, Kyrtopoulos SA, Løvik M, Nielsen JK, Nygaard UC, Pedersen M, Rydberg P, Schoket B, Segerbäck D, Singh R, Sunyer J, Törnqvist M, van Loveren H, van Schooten FJ, Vande Loock K, von Stedingk H, Wright J, Kleinjans JC, Kirsch-Volders M, and van Delft JH

Subjects

Carcinogens toxicity, Child, Cohort Studies, DNA Adducts adverse effects, DNA Adducts analysis, Europe epidemiology, Female, Fetal Blood chemistry, Gene Expression Profiling, Gene Expression Regulation drug effects, Genotype, Hormones adverse effects, Humans, Leukemia chemically induced, Malondialdehyde adverse effects, Malondialdehyde analysis, Micronucleus Tests, Pregnancy, Prenatal Exposure Delayed Effects chemically induced, T-Lymphocytes drug effects, Biomarkers analysis, Carcinogens analysis, Fetal Blood cytology, Hormones analysis, Leukemia epidemiology, Prenatal Exposure Delayed Effects epidemiology, T-Lymphocytes chemistry

Abstract

Background: Leukemia incidence has increased in recent decades among European children, suggesting that early-life environmental exposures play an important role in disease development., Objectives: We investigated the hypothesis that childhood susceptibility may increase as a result of in utero exposure to carcinogens and hormonally acting factors. Using cord blood samples from the NewGeneris cohort, we examined associations between a range of biomarkers of carcinogen exposure and hormonally acting factors with micronuclei (MN) frequency as a proxy measure of cancer risk. Associations with gene expression and genotype were also explored., Methods: DNA and protein adducts, gene expression profiles, circulating hormonally acting factors, and GWAS (genome-wide association study) data were investigated in relation to genomic damage measured by MN frequency in lymphocytes from 623 newborns enrolled between 2006 and 2010 across Europe., Results: Malondialdehyde DNA adducts (M1dG) were associated with increased MN frequency in binucleated lymphocytes (MNBN), and exposure to androgenic, estrogenic, and dioxin-like compounds was associated with MN frequency in mononucleated lymphocytes (MNMONO), although no monotonic exposure-outcome relationship was observed. Lower frequencies of MNBN were associated with a 1-unit increase expression of PDCD11, LATS2, TRIM13, CD28, SMC1A, IL7R, and NIPBL genes. Gene expression was significantly higher in association with the highest versus lowest category of bulky and M1dG-DNA adducts for five and six genes, respectively. Gene expression levels were significantly lower for 11 genes in association with the highest versus lowest category of plasma AR CALUX® (chemically activated luciferase expression for androgens) (8 genes), ERα CALUX® (for estrogens) (2 genes), and DR CALUX® (for dioxins). Several SNPs (single-nucleotide polymorphisms) on chromosome 11 near FOLH1 significantly modified associations between androgen activity and MNBN frequency. Polymorphisms in EPHX1/2 and CYP2E1 were associated with MNBN., Conclusion: We measured in utero exposure to selected environmental carcinogens and circulating hormonally acting factors and detected associations with MN frequency in newborns circulating T lymphocytes. The results highlight mechanisms that may contribute to carcinogen-induced leukemia and require further research.

Published

2014

23. Bulky dna adducts in cord blood, maternal fruit-and-vegetable consumption, and birth weight in a European mother-child study (NewGeneris).

Author

Pedersen M, Schoket B, Godschalk RW, Wright J, von Stedingk H, Törnqvist M, Sunyer J, Nielsen JK, Merlo DF, Mendez MA, Meltzer HM, Lukács V, Landström A, Kyrtopoulos SA, Kovács K, Knudsen LE, Haugen M, Hardie LJ, Gützkow KB, Fleming S, Fthenou E, Farmer PB, Espinosa A, Chatzi L, Brunborg G, Brady NJ, Botsivali M, Arab K, Anna L, Alexander J, Agramunt S, Kleinjans JC, Segerbäck D, and Kogevinas M

Subjects

Female, Humans, Maternal Exposure adverse effects, Polycyclic Aromatic Hydrocarbons toxicity, Birth Weight physiology, DNA Adducts blood, Diet, Fetal Blood chemistry, Fruit, Vegetables

Abstract

Background: Tobacco-smoke, airborne, and dietary exposures to polycyclic aromatic hydrocarbons (PAHs) have been associated with reduced prenatal growth. Evidence from biomarker-based studies of low-exposed populations is limited. Bulky DNA adducts in cord blood reflect the prenatal effective dose to several genotoxic agents including PAHs., Objectives: We estimated the association between bulky DNA adduct levels and birth weight in a multicenter study and examined modification of this association by maternal intake of fruits and vegetables during pregnancy., Methods: Pregnant women from Denmark, England, Greece, Norway, and Spain were recruited in 2006-2010. Adduct levels were measured by the 32P-postlabeling technique in white blood cells from 229 mothers and 612 newborns. Maternal diet was examined through questionnaires., Results: Adduct levels in maternal and cord blood samples were similar and positively correlated (median, 12.1 vs. 11.4 adducts in 108 nucleotides; Spearman rank correlation coefficient = 0.66, p < 0.001). Cord blood adduct levels were negatively associated with birth weight, with an estimated difference in mean birth weight of -129 g (95% CI: -233, -25 g) for infants in the highest versus lowest tertile of adducts. The negative association with birth weight was limited to births in Norway, Denmark, and England, the countries with the lowest adduct levels, and was more pronounced in births to mothers with low intake of fruits and vegetables (-248 g; 95% CI: -405, -92 g) compared with those with high intake (-58 g; 95% CI: -206, 90 g)., Conclusions: Maternal exposure to genotoxic agents that induce the formation of bulky DNA adducts may affect intrauterine growth. Maternal fruit and vegetable consumption may be protective.

Published

2013

24. Dietary acrylamide intake during pregnancy and fetal growth-results from the Norwegian mother and child cohort study (MoBa).

Author

Duarte-Salles T, von Stedingk H, Granum B, Gützkow KB, Rydberg P, Törnqvist M, Mendez MA, Brunborg G, Brantsæter AL, Meltzer HM, Alexander J, and Haugen M

Subjects

Acrylamide pharmacology, Cohort Studies, Female, Hemoglobins chemistry, Humans, Norway, Pregnancy, Surveys and Questionnaires, Acrylamide administration & dosage, Diet, Environmental Exposure, Fetal Development drug effects

Abstract

Background: Acrylamide has shown developmental and reproductive toxicity in animals, as well as neurotoxic effects in humans with occupational exposures. Because it is widespread in food and can pass through the human placenta, concerns have been raised about potential developmental effects of dietary exposures in humans., Objectives: We assessed associations of prenatal exposure to dietary acrylamide with small for gestational age (SGA) and birth weight., Methods: This study included 50,651 women in the Norwegian Mother and Child Cohort Study (MoBa). Acrylamide exposure assessment was based on intake estimates obtained from a food frequency questionnaire (FFQ), which were compared with hemoglobin (Hb) adduct measurements reflecting acrylamide exposure in a subset of samples (n = 79). Data on infant birth weight and gestational age were obtained from the Medical Birth Registry of Norway. Multivariable regression was used to estimate associations between prenatal acrylamide and birth outcomes., Results: Acrylamide intake during pregnancy was negatively associated with fetal growth. When women in the highest quartile of acrylamide intake were compared with women in the lowest quartile, the multivariable-adjusted odds ratio (OR) for SGA was 1.11 (95% CI: 1.02, 1.21) and the coefficient for birth weight was -25.7 g (95% CI: -35.9, -15.4). Results were similar after excluding mothers who smoked during pregnancy. Maternal acrylamide- and glycidamide-Hb adduct levels were correlated with estimated dietary acrylamide intakes (Spearman correlations = 0.24; 95% CI: 0.02, 0.44; and 0.48; 95% CI: 0.29, 0.63, respectively)., Conclusions: Lowering dietary acrylamide intake during pregnancy may improve fetal growth.

Published

2013

25. Birth weight, head circumference, and prenatal exposure to acrylamide from maternal diet: the European prospective mother-child study (NewGeneris).

Author

Pedersen M, von Stedingk H, Botsivali M, Agramunt S, Alexander J, Brunborg G, Chatzi L, Fleming S, Fthenou E, Granum B, Gutzkow KB, Hardie LJ, Knudsen LE, Kyrtopoulos SA, Mendez MA, Merlo DF, Nielsen JK, Rydberg P, Segerbäck D, Sunyer J, Wright J, Törnqvist M, Kleinjans JC, and Kogevinas M

Subjects

Adult, Chromatography, Liquid, Cohort Studies, Diet, Environmental Monitoring, Europe epidemiology, Female, Fetal Blood chemistry, Humans, Infant, Low Birth Weight, Infant, Newborn, Mass Spectrometry, Maternal Exposure, Pregnancy, Prenatal Exposure Delayed Effects chemically induced, Prospective Studies, Regression Analysis, Surveys and Questionnaires, Acrylamide blood, Birth Weight, Environmental Exposure, Environmental Pollutants blood, Epoxy Compounds blood, Head anatomy & histology, Hemoglobins metabolism, Prenatal Exposure Delayed Effects epidemiology

Abstract

Background: Acrylamide is a common dietary exposure that crosses the human placenta. It is classified as a probable human carcinogen, and developmental toxicity has been observed in rodents., Objectives: We examined the associations between prenatal exposure to acrylamide and birth outcomes in a prospective European mother-child study., Methods: Hemoglobin (Hb) adducts of acrylamide and its metabolite glycidamide were measured in cord blood (reflecting cumulated exposure in the last months of pregnancy) from 1,101 singleton pregnant women recruited in Denmark, England, Greece, Norway, and Spain during 2006-2010. Maternal diet was estimated through food-frequency questionnaires., Results: Both acrylamide and glycidamide Hb adducts were associated with a statistically significant reduction in birth weight and head circumference. The estimated difference in birth weight for infants in the highest versus lowest quartile of acrylamide Hb adduct levels after adjusting for gestational age and country was -132 g (95% CI: -207, -56); the corresponding difference for head circumference was -0.33 cm (95% CI: -0.61, -0.06). Findings were similar in infants of nonsmokers, were consistent across countries, and remained after adjustment for factors associated with reduced birth weight. Maternal consumption of foods rich in acrylamide, such as fried potatoes, was associated with cord blood acrylamide adduct levels and with reduced birth weight., Conclusions: Dietary exposure to acrylamide was associated with reduced birth weight and head circumference. Consumption of specific foods during pregnancy was associated with higher acrylamide exposure in utero. If confirmed, these findings suggest that dietary intake of acrylamide should be reduced among pregnant women.

Published

2012

26. Global gene expression analysis in cord blood reveals gender-specific differences in response to carcinogenic exposure in utero.

Author

Hochstenbach K, van Leeuwen DM, Gmuender H, Gottschalk RW, Løvik M, Granum B, Nygaard U, Namork E, Kirsch-Volders M, Decordier I, Vande Loock K, Besselink H, Törnqvist M, von Stedingk H, Rydberg P, Kleinjans JC, van Loveren H, and van Delft JH

Subjects

Acrylamide metabolism, Adult, Biomarkers, Estrogen Receptor alpha genetics, Female, Humans, Male, Micronuclei, Chromosome-Defective statistics & numerical data, Pregnancy, Receptors, Androgen genetics, Sex Characteristics, Signal Transduction, Carcinogens toxicity, Fetal Blood metabolism, Fetus drug effects, Gene Expression Profiling

Abstract

Background: It has been suggested that fetal carcinogenic exposure might lead to predisposition to develop cancer during childhood or in later life possibly through modulation of the fetal transcriptome. Because gender effects in the incidence of childhood cancers have been described, we hypothesized differences at the transcriptomic level in cord blood between male and female newborns as a consequence of fetal carcinogenic exposure. The objective was to investigate whether transcriptomic responses to dietary genotoxic and nongenotoxic carcinogens show gender-specific mechanisms-of-action relevant for chemical carcinogenesis., Methods: Global gene expression was applied in umbilical cord blood samples, the CALUX-assay was used for measuring dioxin(-like), androgen(-like), and estrogen(-like) internal exposure, and acrylamide-hemoglobin adduct levels were determined by mass spectrometry adduct-FIRE-procedure(TM). To link gene expression to an established phenotypic biomarker of cancer risk, micronuclei frequencies were investigated., Results: While exposure levels did not differ between sexes at birth, important gender-specific differences were observed in gene expressions associated with these exposures linked with cell cycle, the immune system and more general cellular processes such as posttranslation. Moreover, oppositely correlating leukemia/lymphoma genes between male and female newborns were identified in relation to the different biomarkers of exposure that might be relevant to male-specific predisposition to develop these cancers in childhood. CONCLUSIONS/IMPACT: This study reveals different transcriptomic responses to environmental carcinogens between the sexes. In particular, male-specific TNF-alpha-NF-kB signaling upon dioxin exposure and activation of the Wnt-pathway in boys upon acrylamide exposure might represent possible mechanistic explanations for gender specificity in the incidence of childhood leukemia., (2012 AACR)

Published

2012

27. Analysis of hemoglobin adducts from acrylamide, glycidamide, and ethylene oxide in paired mother/cord blood samples from Denmark.

Author

von Stedingk H, Vikström AC, Rydberg P, Pedersen M, Nielsen JK, Segerbäck D, Knudsen LE, and Törnqvist M

Subjects

Adult, Case-Control Studies, Chromatography, Liquid, Denmark, Female, Fetal Blood chemistry, Fetus, Humans, Mass Spectrometry, Maternal Exposure, Placenta physiology, Pregnancy, Smoking adverse effects, Acrylamide blood, Epoxy Compounds blood, Ethylene Oxide blood, Hemoglobins metabolism, Smoking blood

Abstract

The knowledge about fetal exposure to acrylamide/glycidamide from the maternal exposure through food is limited. Acrylamide, glycidamide, and ethylene oxide are electrophiles and form adducts with hemoglobin (Hb), which could be used for in vivo dose measurement. In this study, a method for analysis of Hb adducts by liquid chromatography-mass spectrometry, the adduct FIRE procedure, was applied to measurements of adducts from these compounds in maternal blood samples (n = 87) and umbilical cord blood samples (n = 219). The adduct levels from the three compounds, acrylamide, glycidamide, and ethylene oxide, were increased in tobacco smokers. Highly significant correlations were found between cord and maternal blood with regard to measured adduct levels of the three compounds. The mean cord/maternal hemoglobin adduct level ratios were 0.48 (range 0.27-0.86) for acrylamide, 0.38 (range 0.20-0.73) for glycidamide, and 0.43 (range 0.17-1.34) for ethylene oxide. In vitro studies with acrylamide and glycidamide showed a lower (0.38-0.48) rate of adduct formation with Hb in cord blood than with Hb in maternal blood, which is compatible with the structural differences in fetal and adult Hb. Together, these results indicate a similar life span of fetal and maternal erythrocytes. The results showed that the in vivo dose in fetal and maternal blood is about the same and that the placenta gives negligible protection of the fetus to exposure from the investigated compounds. A trend of higher levels of the measured adducts in cord blood with gestational age was observed, which may reflect the gestational age-related change of the cord blood Hb composition toward a higher content of adult Hb. The results suggest that the Hb adduct levels measured in cord blood reflect the exposure to the fetus during the third trimester. The evaluation of the new analytical method showed that it is suitable for monitoring of background exposures of the investigated electrophilic compounds in large population studies.

Published

2011

28. A new modified Edman procedure for analysis of N-terminal valine adducts in hemoglobin by LC-MS/MS.

Author

von Stedingk H, Rydberg P, and Törnqvist M

Subjects

Calibration, Fluorescein-5-isothiocyanate chemistry, Reference Standards, Chromatography, High Pressure Liquid methods, Hemoglobins chemistry, Tandem Mass Spectrometry methods, Valine analysis

Abstract

A rapid and sensitive method using liquid chromatography-tandem mass spectrometry (LC-MS/MS) for simultaneous determination of adducts from acrylamide, glycidamide and ethylene oxide to N-terminal valines in hemoglobin (Hb) was developed. This new procedure is based on the same principles as the N-alkyl Edman procedure for analysis of adducts from electrophilic agents to N-terminal valines in Hb. The N-substituted valines can be detached, enriched and measured selectively as thiohydantoins by the use of an Edman reagent, in this case fluorescein isothiocyanate (FITC). This procedure is denoted as the "adduct FIRE procedure" as the FITC reagent is used for measurement of adducts (R) formed from electrophilic compounds with a modified Edman procedure. In this study, fluorescein thiohydantoin (FTH) analytes of N-substituted valines from acrylamide, glycidamide and ethylene oxide, as well as their corresponding hepta- and tri-deuterium-substituted analogues, were synthesized. These analytes (n=8) were then characterized by LC-MS/MS (ESI, positive ion mode) and obtained product ions were interpreted. A considerable work with optimization of the FIRE procedure™, resulted in a procedure in which low background levels of the studied adducts could be measured from 250 μL lyzed whole blood samples (human non-smokers). The analytes were enriched and purified with solid phase extraction columns and analyzed by LC-MS/MS with LOQ down to 1 pmol adduct/gHb. Compared to other procedures for determination of N-terminal Hb adducts, the introduction of FITC has led to a simplified procedure, where whole blood also can be used, giving new opportunities and reduced hand on time with increased sample throughput., (Copyright © 2010 Elsevier B.V. All rights reserved.)

Published

2010

29. Methyl vinyl ketone--identification and quantification of adducts to N-terminal valine in human hemoglobin.

Author

von Stedingk H, Davies R, Rydberg P, and Törnqvist M

Subjects

Calibration, Chromatography, Gas methods, Chromatography, Liquid methods, Fluorescein-5-isothiocyanate, Fluorescent Dyes, Humans, Tandem Mass Spectrometry methods, Butanones analysis, Hemoglobins chemistry, Valine chemistry

Abstract

Adducts to N-terminal valines in Hb have been shown useful as biomarkers of exposure to electrophilic compounds. Adducts from many compounds have earlier been measured with a modified Edman degradation method using a GC-MS/MS method. A recently developed method, the adduct FIRE procedure™, adopted for analysis by LC-MS/MS, has been applied in this study. With this method a fluorescein isothiocyanate (FITC) reagent is used to measure adducts (R) from electrophiles with a modified Edman procedure. By using LC-MS/MS in product ion scan mode, a new peak was identified and the obtained MS data indicated that this adduct could originate from methyl vinyl ketone (MVK). Incubation of human-, sheep- and bovine blood with MVK increased the signal of the identified peak. By comparing the LC-MS/MS data from the unknown background peak with data obtained from synthesized fluorescein thiohydantoin (FTH) standards of the MVK adduct to valine and d(8)-valine, the identity of this adduct was confirmed. The MVK adduct was shown present in human blood (∼35 pmol/g globin, n=3) and only just above LOD in bovine blood, n=1 (LOD=2 pmol/g globin). MVK reacts, in similarity with acrylamide, via Michael addition. MVK is known to occur in the environment and has earlier been observed in biological samples, which means that there are possible natural and anthropogenic exposure sources. Analysis of an Hb adduct from MVK in humans has to our knowledge not been described before., (Copyright © 2010 Elsevier B.V. All rights reserved.)

Published

2010

30. LC/MS/MS Analysis of N-Terminal Protein Adducts with Improved Sensitivity: A Comparison of Selected Edman Isothiocyanate Reagents.

Author

Rydberg P, von Stedingk H, Magnér J, and Björklund J

Abstract

This study provides a basis for a new and straightforward method for LC/MS/MS-based screening of N-terminal protein adducts. This procedure is denoted the "FIRE procedure" as fluorescein isothiocyanate (FITC) gave superior sensitivity by LC/MS/MS when measuring adducts (R) of electrophilic compounds with a modified Edman procedure. The principles of the FIRE-procedure are that adducts to N-terminal amino acids selectively are detached and measured from of proteins after derivatisation by isothiocyanate Edman reagents. In this study, FITC, 4-N,N-dimethylaminoazobenzene 4'-isothiocyanate (DABITC) and 4-dimethylamino-1-naphthyl isothiocyanate (DNITC) were used to synthesize thiohydantoin analytes from valine and N-methylvaline. The sensitivity by LC/MS/MS was enhanced by up to three orders of magnitude as compared to phenyl isothiocyanate and higher as compared to pentafluorophenyl isothiocyanate. The FITC reagent will enable measurements of low background adduct levels. Synthesized analytes were characterised with, for example, (1)H NMR, (13)C NMR, LC/MS/MS, and UV.

Published

2009