Abstract:
:Dimethylacetamide (DMAc) is a skin-penetrating solvent able to induce hepatic damage after chronic exposure. Previous research has indicated that metabolism may be saturated at its present TLV/TWA (10 ppm). Biological monitoring of monomethylacetamide (MMAc), the primary metabolite of DMAc, might therefore underestimate exposure to DMAc and related health hazards. We used the recirculating perfusion technique in isolated rat liver to evaluate DMAc metabolism. Medium concentrations starting at about 30, 50, 100 and 275 microM, respectively, were tested. Perfusate samples were taken regularly and analysed for DMAc; pharmacokinetic parameters (extraction ratio and clearance) were calculated for each perfusion. Inlet DMAc concentrations were calculated and concentration groups divided in 16, 36, 70, 160, 225 microM. The extraction ratio of the 16 microM group differed significantly from the other concentration groups tested. DMAc metabolism was saturated at a DMAc concentration of 36 microM. Extraction ratios were unaffected when cimetidine, an inhibitor of cytochrome P450 activity, was added to the perfusion medium or when cimetidine-pretreated animals were used. DMAc clearance was 2.20 ml min-1 at a medium concentration of about 36 microM. Extrapolation of the observed (rat) liver clearance to man showed that airborne concentrations of 18 ppm would, under the presumptions used, lead to saturated metabolism of DMAc; however, saturation at even lower concentrations could not be excluded.
journal_name
Hum Exp Toxicoljournal_title
Human & experimental toxicologyauthors
Palmen NG,Evelo CT,Borm PJ,Henderson PTdoi
10.1177/096032719301200206subject
Has Abstractpub_date
1993-03-01 00:00:00pages
127-33issue
2eissn
0960-3271issn
1477-0903journal_volume
12pub_type
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