| Literature DB >> 15513896 |
Beom Soo Shin1, Chul Hwan Kim, Yoon Sik Jun, Dong Hwan Kim, Byung Mu Lee, Chi Ho Yoon, Eun Hye Park, Kang Choon Lee, Soon-Young Han, Kui Lea Park, Hyung Sik Kim, Sun Dong Yoo.
Abstract
A physiologically based pharmacokinetic (PBPK) model consisting of vein, artery, lung, liver, spleen, kidneys, heart, testes, muscle, brain, adipose tissue, stomach, and small intestine was developed to predict the tissue distribution and blood pharmacokinetics of bisphenol A in rats and humans. To demonstrate the validity of the developed PBPK model, bisphenol A was administered to rats by multiple iv injections to steady state. The PBPK model predicted the steady-state levels of bisphenol A in blood and various tissues observed in rats after multiple iv injections. The PBPK model was further applied to predict blood and various tissue levels of bisphenol A in a 70 kg-human after single iv injection (5-mg dose) and multiple oral administrations to steady state (100-mg doses every 24 h). The simulated steady-state human blood levels (0.9-1.6 ng/ml) were comparable to basal blood levels of bisphenol A reported in literature (1.49 ng/ml). Furthermore, pharmacokinectic parameters of CL (116.6 L/h), Vss (141.8 L), and t1/2 (76.8 min) predicted for humans were comparable to those previously predicted by simple allometric scaling. This PBPK model may provide insights into the tissue distribution characteristics as a result of human exposure to bisphenol A.Entities:
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Year: 2004 PMID: 15513896 DOI: 10.1080/15287390490514615
Source DB: PubMed Journal: J Toxicol Environ Health A ISSN: 0098-4108