Pregnancy Clinical Trial
Official title:
Transplacental Transfer of Drugs Used in Pregnant Women
The most important guideline for drug prescription concerning pregnant women is 'drugs
should be given only if the maternal benefits outweigh the potential risk to the fetus'.
However, poor data is available on maternal drug disposition and transfer through the
placenta, so the evidence available for decision making in clinical practice is weak.
An ex-vivo placenta perfusion model will be used to explore the mechanisms governing
differences between fetal and maternal drug exposure. The expression of placental
transporters and cytochrome P450 (CYP) enzymes will be investigated in primary placenta cell
culture and placental biopsies from different gestational stages to learn how the placental
drug transfer and disposition is regulated.
The investigators choose to examine the transfer of paracetamol, erythromycin and
azithromycin because these drugs are commonly used in human pregnancies and have different
metabolic pathways.
1. Background While many drugs are administered to pregnant women, only poor data exist to
determine a therapeutically optimal and safe drug treatment in this patient population.
The general advise on the use of medicines in pregnancy is that you can only prescribe
drugs to pregnant women if the benefits for the mother outweigh the risks for the
fetus. The problem is that for most medicines safety data are lacking. Most drug
effects are dose dependent. So the first step to examine potential fetotoxicity is to
test transplacental transfer of drugs.
Placental transfer from the maternal to the fetal side occurs primarily via passive
diffusion, the physicochemical properties of drugs such as lipid solubility, polarity
and molecular weight primarily determine the rate of transfer across the placenta.
According to membrane permeability properties, low-molecular-weight, lipid-soluble,
unbound and unionized compounds can easily cross the human placenta. In addition, some
drugs are pumped across the placenta by various active transporters located on both the
fetal and maternal side of the trophoblast layer. The most important transporters are
P-glycoprotein (P-gp, encoded by the multidrug resistance (MDR)1 gene), Breast cancer
resistance protein (BCRP) and multidrug resistance-associated protein (MRP) 1-3 and 5.
The transfer of foreign chemicals across the placenta can also be modified by
metabolism in the placenta itself. The human placenta contains multiple enzyme systems,
like CYP2E1 and CYP3A4.
2. Aim & methods:
The aim of this study is to determine fetal drug concentrations of paracetamol, erythromycin
and azithromycin by transplacental transport in an ex-vivo placenta perfusion model.
Simultaneously collected maternal and fetal drug plasma levels will be compared to assess
fetal drug levels based on maternal drug plasma levels.
Moreover, the transporter and metabolizing activity of the trophoblast cells will be
examined in a primary human trophoblast culture, and expression of enzymes and transporters
will be evaluated at different gestational ages in human placenta biopsies.
Medicines: The investigators choose to examine the transfer of paracetamol, erythromycin and
azithromycin because these drugs are commonly used in human pregnancies.
Since the ORACLE trial, erythromycin is in Belgium the first choice treatment in patients
with preterm rupture of membranes, despite the fact that the pharmacokinetics (PK) of this
drug has been hardly studied in pregnant women. Erythromycin is unstable under acidic
conditions while azithromycin is a semi-synthetic macrolide, with a better gastro-intestinal
tolerability and tissue penetration than erythromycin and an excellent activity against
sexually transmitted pathogens, especially Chlamydia trachomatis. Because of these
characteristics more physicians start to switch to azithromycin even without PK data
available in pregnancy.
Paracetamol (acetaminophen) is used as first choice painkiller in pregnancy, but also for
this drug surprisingly few PK data are available.
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