1995
DOI: 10.2307/3432865
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A Pharmacokinetic Model of Inhaled Methanol in Humans and Comparison to Methanol Disposition in Mice and Rats

Abstract: (Perkins et al., submitted). Elimination via the lungs (after exposure) and the kidney is theoretically a small fraction of total methanol elimination (8,11) and modeled well in both rat and mouse without being specifically included (10). In both the rat and mouse, the systemic disposition of methanol was similar after oral (PO), intravenous (IV), or inhalation administration (Perkins et al., submitted).To assess risk to the human conceptus based on extrapolation from rodent data, it is desirable to begin with… Show more

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“…Correspondingly, a blood level of 5 mg/dl for any period might then be taken as the maximum ''safe'' level, i.e., one unlikely to be associated with toxic effects. 10,12,19,22 23 Literature review to obtain pharmacokinetic model…”
Section: Maximum Tolerable Blood Levelmentioning
confidence: 99%
“…Correspondingly, a blood level of 5 mg/dl for any period might then be taken as the maximum ''safe'' level, i.e., one unlikely to be associated with toxic effects. 10,12,19,22 23 Literature review to obtain pharmacokinetic model…”
Section: Maximum Tolerable Blood Levelmentioning
confidence: 99%