Drugs in Pregnancy & Lactation
Placental Transfer, Teratogenesis, Gestational Pharmacokinetics, Drug Use in Lactation & Risk Labelling
Past RGUHS · 10
RGUHSDec '23
RGUHSJul '23
RGUHSNov '22
RGUHSMay '22
RGUHSMay '19
RGUHSNov '18
RGUHSOct '10
RGUHSOct '08
RGUHSSep '07
RGUHSApr '06
Introduction & guiding principles
- Pregnancy is the "last true therapeutic orphan" — ethical, medicolegal and fetal-safety concerns mean almost no drug trials are done in pregnant women, so most labels carry "no adequate well-controlled studies… use only if clearly needed."
- The clinician's core task is a risk–benefit balance: fetal drug risk (chiefly teratogenesis) is weighed against the risk to mother and fetus of the untreated maternal disease — the latter is often wrongly omitted, leaving pregnant women under-treated.
- Indian PG framing — drugs should generally be avoided; if required, used cautiously balancing risk vs benefit for both — for many diseases one or two agents are known to be reasonably safe (e.g. methyldopa for hypertension, chloroquine for malaria).
- Baseline (background) risk — even with no teratogenic exposure, the population risk of a major congenital malformation is ~3% (3–5%); minor anomalies add 7–14%. Drugs cause <1% of all birth defects (~65–80% unknown cause, ~15% chromosomal); fewer than 30 drugs are proven human teratogens.
- Counselling matters — ~50% of pregnancies are unplanned and patients often assume every drug is a teratogen; evidence-based counselling demonstrably prevents unnecessary terminations.
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Drugs In Pregnancy Lactation
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