Determination of in vitro metabolic hepatic clearance of valproic acid (VPA) and five analogues by UPLC-MS-QTOF, applicable in alternatives to animal testing.
Laboratory measurements of intrinsic clearance support the development of TK models, with potential relevance
to weight of evidence toxicity assessments of xenobiotics, including read-across, the concept of predictive estimation
by data extrapolation between chemicals of similar structure (analogues).
In this work a procedure with analytical method for determination of in vitro hepatic metabolic clearance,
relevant to biotransformation toxicokinetic (TK) modelling, is presented. Cryopreserved primary human hepatocytes
represent a suitable cells, due to their biological characteristics, for providing an in vitro model for
simulating in vivo metabolic clearance.
The experimental part considered an adequate sequential time-frame for collecting samples and controls for all
chemicals tested, including centrifugation and aliquoting of the corresponding fractions until the instrumental
session.
For the first time, in vitro hepatocyte intrinsic clearance was measured for six analogue test chemicals: valproic
acid, 2-ethyl caproic acid, octanoic acid, valeric acid, 2-methyl butyric acid and 2-trans pentenoic acid, during
incubated cell culture exposure up to 2 h or 3.5 h. The time dependence of any metabolism was determined from
analysis of the supernatant at intervals using a new developed analytical method for UPLC coupled with QTOF
mass spectrometer. The chemicals could then be ranked by their relative intrinsic clearance.
The analyses were reproducible, with coherence of the calculated in vitro intrinsic clearance between
experiments.
FORTANER TORRENT Salvador;
MENDOZA Emilio;
COLE Thomas;
LOSTIA Alfonso;
2021-09-21
ELSEVIER
JRC125809
1570-0232 (online),
https://www.sciencedirect.com/science/article/pii/S1570023221003743?via%3Dihub,
https://publications.jrc.ec.europa.eu/repository/handle/JRC125809,
10.1016/j.jchromb.2021.122893 (online),
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