תקציר
The immunosuppressant azathioprine is increasingly being used in pregnancy. The human placenta is considered a relative barrier to the major metabolite, 6-mercaptopurine (6-MP), and likely explains the lack of proven teratogenicity in humans. The aim of this study was to determine how the human placenta restricts 6-MP transfer using the human placental perfusion model. After addition of 50. ng/ml (n=4) and 500. ng/ml (n=3) 6-MP into the maternal circulation, there was a biphasic decline in its concentration and a delay in fetal circulation appearance. Under equilibrative conditions, the fetal-to-maternal concentration ratio was >1.0 as a result of ion trapping. Binding to placental tissue and maternal pharmacokinetic parameters are the main factors that restrict placental transfer of 6-MP. Active transport is unlikely to play a significant role and drug interactions involving, or polymorphisms in, placental drug efflux transporters are not likely to put the fetus at risk of higher 6-MP exposure.
שפה מקורית | אנגלית |
---|---|
עמודים (מ-עד) | 349-353 |
מספר עמודים | 5 |
כתב עת | Reproductive Toxicology |
כרך | 32 |
מספר גיליון | 3 |
מזהי עצם דיגיטלי (DOIs) | |
סטטוס פרסום | פורסם - נוב׳ 2011 |
פורסם באופן חיצוני | כן |