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Aquatic ecosystems continue to be threatened by chemical pollution. To what extent organisms are able to cope with chemical exposure depends on their ability to display mechanisms of defense across different organs. Among these mechanisms, biotransformation processes represent key physiological responses that facilitate detoxification and reduce the bioaccumulation potential of chemicals. Biotransformation does not only depend on the ability of different organs to display biotransformation enzymes but also on the affinity of chemicals towards these enzymes. In the present study, we explored the ability of different organs and of two freshwater fish to support biotransformation processes through the determination of in vitro phase I and II biotransformation enzyme activity, and their role in supporting intrinsic clearance and the formation of biotransformation products. Three environmentally relevant pollutants were evaluated: the polycyclic aromatic hydrocarbon (PAH) pyrene (as recommended by the OECD 319b test guideline), the fungicide azoxystrobin, and the pharmaceutical propranolol. Comparative studies using S9 sub -cellular fractions derived from the liver, intestine, gills, and brain of brown trout ( Salmo trutta ) and rainbow trout ( Oncorhynchus mykiss ) revealed significant phase I and II enzyme activity in all organs. However, organ- and species -specific differences were found. In brown trout, significant extrahepatic biotransformation was observed for pyrene but not for azoxystrobin and propranolol. In rainbow trout, the brain appeared to biotransform azoxystrobin. In this same species, propranolol appeared to be biotransformed by the intestine and gills. Biotransformation products could be detected only from hepatic biotransformation, and their profiles and formation rates displayed species -specific patterns and occurred at different magnitudes. Altogether, our findings further contribute to the current understanding of organ -specific biotransformation capacity, beyond the expression and activity of enzymes, and its dependence on specific enzyme -chemical interactions to support mechanisms of defense against exposure.
Giovanni De Cesare, Paolo Perona, Giulio Calvani, Francesca Padoan
Giovanni De Cesare, Robin Schroff, Camille Blanck