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Comprehensive Toxicology 2010
DOI: 10.1016/b978-0-08-046884-6.01029-0
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Thioacetamide

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Cited by 4 publications
(1 citation statement)
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“…The hepatotoxic properties of TAA in mice and rats induces oxidative stress resulting first in formation of intracellular lipid deposits in the liver parenchymal cells (hepatocyte ballooning), and later leading to HEPs damage and necrosis [ 62 ]. Bioactivation of TAA into its hepatotoxic counterpart, TASO 2 [ 63 ], requires proteins from the cytochrome p450 complex, functional orthologs for many of which exist in zebrafish, including proteins with > 44.87% sequence similarity to CYP2E1, the protein thought to be directly responsible for TAA metabolism in humans [ 64 ]. Moreover, CYP2E1 function was reproduced in zebrafish tissue homogenates, albeit without identifying the specific enzyme responsible for the process [ 65 ].…”
Section: Discussionmentioning
confidence: 99%
“…The hepatotoxic properties of TAA in mice and rats induces oxidative stress resulting first in formation of intracellular lipid deposits in the liver parenchymal cells (hepatocyte ballooning), and later leading to HEPs damage and necrosis [ 62 ]. Bioactivation of TAA into its hepatotoxic counterpart, TASO 2 [ 63 ], requires proteins from the cytochrome p450 complex, functional orthologs for many of which exist in zebrafish, including proteins with > 44.87% sequence similarity to CYP2E1, the protein thought to be directly responsible for TAA metabolism in humans [ 64 ]. Moreover, CYP2E1 function was reproduced in zebrafish tissue homogenates, albeit without identifying the specific enzyme responsible for the process [ 65 ].…”
Section: Discussionmentioning
confidence: 99%