A Textbook of Clinical Pharmacology and Therapeutics

an anti-analgesic effect when combined with pethidine), and
naloxone(an opioid antagonist) must always be available.
Respiratory depression in the newborn is not usually a prob-
lem with modern general anaesthetics currently in use in
Caesarean section. Several studies have shown an increased
incidence of spontaneous abortions in mothers who have had
general anaesthesia during pregnancy, although a causal rela-
tionship is not proven, and in most circumstances failure to
operate would have dramatically increased the risk to mother
and fetus.

ANTI-EMETICS

Nausea and vomiting are common in early pregnancy, but are
usually self-limiting, and ideally should be managed with
reassurance and non-drug strategies, such as small frequent
meals, avoiding large volumes of fluid and raising the head of
the bed. If symptoms are prolonged or severe, drug treatment
may be effective. An antihistamine, e.g. promethazineor
cyclizinemay be required. If ineffective, prochlorperazineis
an alternative. Metoclopramideis considered to be safe and
efficacious in labour and before anaesthesia in late pregnancy,
but its routine use in early pregnancy cannot be recommended
because of the lack of controlled data, and the significant inci-
dence of dystonic reactions in young women.

DYSPEPSIA AND CONSTIPATION

The high incidence of dyspepsia due to gastro-oesophageal
reflux in the second and third trimesters is probably related to
the reduction in lower oesophageal sphincter pressure. Non-
drug treatment (reassurance, small frequent meals and advice
on posture) should be pursued in the first instance, particu-
larly in the first trimester. Fortunately, most cases occur later
in pregnancy when non-absorbable antacids, such as algi-
nates, should be used. In late pregnancy, metoclopromideis
particularly effective as it increases lower oesophageal sphinc-
ter pressure. H 2 -receptor blockers should not be used for non-
ulcer dyspepsia in this setting. Constipation should be managed
with dietary advice. Stimulant laxatives may be uterotonic
and should be avoided if possible.

PEPTIC ULCERATION

Antacids may relieve symptoms. Cimetidineandranitidine
have been widely prescribed in pregnancy without obvious
damage to the fetus. There are inadequate safety data on the
use of omeprazoleor other proton pump inhibitors in preg-
nancy. Sucralfatehas been recommended for use in preg-
nancy in the USA, and this is rational as it is not systemically
absorbed.Misoprostol, a prostaglandin which stimulates the
uterus, is contraindicated because it causes abortion.

ANTI-EPILEPTICS

Epilepsy in pregnancy can lead to fetal and maternal morbid-

ity/mortality through convulsions, whilst all of the anticon-

vulsants used have been associated with teratogenic effects

(e.g.phenytoinis associated with cleft palate and congenital

heart disease). However, there is no doubt that the benefits of

good seizure control outweigh the drug-induced teratogenic

risk. Thorough explanation to the mother, ideally before a

planned pregnancy, is essential, and it must be emphasized

that the majority (90%) of epileptic mothers have normal

babies. (The usual risk of fetal malformation is 2–3% and in

epileptic mothers it is up to 10%.) In view of the association of

spina bifida with many anti-epileptics, e.g. sodium valproate

andcarbamazepinetherapy, it is often recommended that the

standard dose of folic acid should be increased to 5 mg daily.

Both of these anti-epileptics can also cause hypospadias. As

in non-pregnant epilepsy, single-drug therapy is preferable.

Plasma concentration monitoring is particularly relevant for

phenytoin, because the decrease in plasma protein binding and

the increase in hepatic metabolism may cause considerable

changes in the plasma concentration of free (active) drug. As

always, the guide to the correct dose is freedom from fits and

absence of toxicity. Owing to the changes in plasma protein

binding, it is generally recommended that the therapeutic

range is 5–15 mg/L, whereas in the non-pregnant state it is

10–20 mg/L. This is only a rough guide, as protein binding

varies.

The routine injection of vitamin K recommended at birth

counteracts the possible effect of some anti-epileptics on

vitamin K-dependent clotting factors.

Magnesium sulphate is the treatment of choice for the pre-

vention and control of eclamptic seizures.

PRESCRIBING INPREGNANCY 49

Key points

• Epilepsy in pregnancy can lead to increased fetal
  and maternal morbidity/mortality.


• All anticonvulsants are teratogens.


• The benefits of good seizure control outweigh
  drug-induced teratogenic risk.


• Give a full explanation to the mother (preferably
  before pregnancy): most epileptic mothers (90%)
  have normal babies.


• Advise an increase in the standard dose of folic acid up
  to 12 weeks.


• Make a referral to the neurologist and obstetrician.


• If epilepsy is well controlled, do not change
  therapy.


• Monitor plasma concentrations (levels tend to fall,
  and note that the bound: unbound ratio changes); the
  guide to the correct dose is freedom from fits and
  absence of toxicity.


• An early ultrasound scan at 12 weeks may detect gross
  neural tube defects.


• Detailed ultrasound scan and α-fetoprotein at 16–18
  weeks should be considered.