3. Drug use during Pregnancy
• Every system in the body is affected by
pregnancy
• Pharmacokenetics & pharmacodynamics of
drugs is affected by pregnancy
• At present these pharmacokinetic factors are
beginning to be understood whereas
pharmacodynamics information is still
incomplete
3
4. • 1. Absorption: ↑ed
Gastric emptying time is delayed & gut motility
reduced because of ↑ed progesterone
Vasodilation , tissue perfusion ↑ed
• 2. Distribution: ↑ed
Total body water increases i.e. hemodilution
Plasma albumin conc. ↓ed so ↑ed free drug
conc.
Increased body fat, reservoir of lipid soluble drug
Pharmacokenetics Of Drugs During
Pregnancy
4
5. • 3. Metabolism:
hepatic metabolism increases but no altered
hepatic blood flow
• 4. Elimination:
Renal blood flow doubles, so rapid
elimination of drugs excreted by kidney
(e.g.Aminoglycosides)
Dose should be increased in such cases
Pharmacokenetics Of Drugs During
Pregnancy
5
6. Factors Affecting Placental Drug
Transfer & Subsequent Effect On Fetus
1. Physiochemical properties of the drug
2. Rate at which drug crosses placenta & amount
reaching the fetus
3. Duration of exposure to drug
4. Distribution characteristics of drug in different
fetal tissues
5. Stage of placental & fetal development at the
time of exposure
6. Effects of drugs used in combination
6
7. A. Lipid solubility
Lipophilic drugs crosses placenta more
e.g.thiopental may cause apnoea in fetus,
salicylate is ionised but very lipid soluble
B. Molecular size & pH
250-500 easily
500-1000 with difficulty
>1000 poorly
maternal blood pH 7.4 & fetal 7.3 , may lead to ion
trapping in c/o pKa >7.4
C. Placental transporters
e.g. P glycoprotein transporter encoded by MDR1
gene pumps back some drugs like cancer drugs
(doxorubicin)
and viral protease inhibitors
7
8. D. Protein binding
more protein bound drug crosses less
doesn’t affect lipid soluble drug that much
differential protein binding – Glyburide
E. Placental & fetal drug metabolism
1) Placenta: aromatic oxidation reactions occur
e.g. Phenobarbital
may also lead to toxic metabolite e.g. ethanol,
benzpyrenes
2) Fetus: 40-60% blood enters fetal liver
a proportion of blood is shunted back
through placenta
8
9. Pharmacodynamics
A. Maternal Drug Actions
• Effect on reproductive tissue may be altered
by endocrinal environment due to pregnancy
• Effect on other tissues not changed much
• Altered physiologic context may require
treatment
e.g. cardiac glycosides & diuretics for heart
failure , insulin for pregnancy induced
diabetes
9
10. B. Therapeutic Drug Actions In The Fetus
emerging area ‘ Fetal Therapeutics’
i. Corticosteroids: e.g. dexamethasone for lung
maturation in premature labour
ii. Phenobarbitone: for neonatal jaundice or
decrease intra cranial bleeding
iii. Zidovudine or nevirapine: alone or in
combination to prevent vertical transmission
Pharmacodynamics
10
11. Toxic Effects Of Drugs On The Embryo,
Fetus, Or Neonate
May vary
• No effect.
• Little
• Serious- fetal toxicity
• Spontaneous abortion
• Death
• Fetal malfunction
• Fetal malformations.
11
12. C. Predictable Toxic Effects
i. Opioids : dependance , neonatal withdrawal
syndrome, respiration depression
ii. ACE inhibitors : renal damage
iii. Diethylstilbestrol: adenocarcinoma of vagina
after puberty
Pharmacodynamics
12
13. D. Teratogenic Drug Actions:
Birth Defects
• Incidence of major structural
defects(abnormalities) is about 6% of all
pregnancies.
• 3% are caused by drugs or environmental
factors/exposure
• 3% have a genetic or unknown causes
Pharmacodynamics
13
14. • 1/2 of the birth defects are obvious at birth.
• 1/2 of the birth defects aren’t discovered until
later in life or discovered during an autopsy
• Incidence of minor structural anomalies is not
known.
• Incidence of functional abnormalities is not
known-growth restrictions, mental
retardation, and learning disabilities
• Some abnormalities have multiple causes-
genetic factors, environmental factors,
chemicals or drugs.
14
15. Teratogenic
Teratogenesis
• Teras-”monster”
• Gensis-”producing”
• Birth defects/distortion of gross anatomy.
• Examples- cleft lip/palate, clubfoot, neural tubal
defects, missing or malformed limbs/fingers.
• Now also- behavioral and/ or biochemical and/or
physiological abnormalities.
• Death of fetus & carcinogenic effect
15
16. Mechanism of Teratogenesis
• Direct effect on maternal tissue with secondary
effect on fetus
• Indirect-such as interfering with o2 or nutrients.
• Teratogenesis maybe direct-malformations of
structures. e.g.
i. Vitamin A analogs (isotretinoin,etretinate)
ii. Deficiency of a critical substance (folic acid
causing neural tube defects)
iii. Continues exposure to teratogen may produce
cumulative effect (Fetal Alcohol Syndrome)
16
17. Proving A Drug Is A Teratogen
3 Criteria must be met:
• 1. Drug must cause a characteristic set of
malformations with selectivity for certain
organs
• 2. It must act only during a specific window of
vulnerability (organogenesis of target organ)
• 3. The incidence of malformations should
increase with increased dosage & duration of
exposure.
17
18. Fetal Effects From Drugs Depend On
Several Factors
• Time- when drug is taken in pregnancy.
• Preimplantation/presomite period-
conception to 2 week
• High dose- maybe lethal/death/abortions.
• Low dose-maybe nothing.
As per time …..
18
19. ① 0-2 weeks-period of dividing zygote ,
implantation
• Prenatal death may occur
• Abortion may occur due to oxytosics e.g. ergot
alkaloids, anti metabolites
② Embryonic period-3-8 weeks - First trimester
• Gross malformations
• E.G. One time exposure to thalidomide through
4th to 7th week-causes missing limbs(phocomalia).
③Fetal period-9-40 weeks(term)
• Function problems rather than gross anatomy
• Learning deficits &/or behavioral abnormalities
19
25. Others such as
• Thrombocytopenia due to sensitization by
thiazide diuretics when given to mother
• Mercury may cause impaired brain
development , cerebral palsy, mental
retardation etc.
• Other fetal defects due to effect of drug on
spermatogenesis are suspected
25
26. Why is identification of teratogenic
agents sometimes difficult to
identify?
• Incidence of congenital anomalies is generally
low.
• Animal tests may not be reliable
• Prolonged or increased exposure maybe
required.
• Effects maybe delayed or not reconized.
• Behavioral effects are difficult to document.
• Controlled experiments cannot be done on
humans.
26
27. • Documentation is incomplete
• Only in a limited number of drugs is the
teratogenic effects known or proven.
• Lack of proof of teratogenicity does not
mean a drug is safe in pregnancy
• May mean there is a lack of research or
information.
27
28. How Is Data Collected On Drugs
Which Cause Problems In
Pregnancies?
• No human experimentation
• Systematic collection and analyzing of data
on drugs taken by pregnant clients.
• Reporting of information by health
professionals.
28
30. Precautions While Prescribing During
Reproductive Age & Pregnancy
1. In c/o contraception failure – Explain risk of drug
already received & to continue pregnancy or
abort
2. Similarly, in c/o post coital contraception
3. If a woman is being treated , explain risks to
fetus & advise to avoid pregnancy till therapy
completes
4. If a woman of reproductive age comes with any
ailment pregnancy should be ruled out & then
follow guideline as shown next
30
31. A. If not pregnant
i) Conception not desired : normal treatment
ii) Conception desired:
• Advise not to take any medication after last
menstrual period
• Advise folic acid & iron supplements
• If diabetic start her on insulin
• Avoid self treatment if ill, consult doctor
31
32. B. If pregnant
• Advise same as 4.A.ii in last slide
• Avoid use of drug & treat minor problems
without drugs
• Strictly avoid proven teratogens i.e. Cat. X & D
• If required prescribe proven safe drug
• Use minimal dose for shortest period of time
• If an unsafe or unproven drug has to be used
than do α-fetoproteins at 16 weeks of
gestation & high quality ultrasound at 18
weeks to asses anomalies
32
33. Education Of Pregnant/Pre-pregnant
• Provide accurate information with rationales
• Information should be current and based on evidence.
• Establish environment conducive to exchange of
information - trust.
• Potential harm/risks. Common substances & OTC drugs
to avoid in pregnancy- ASA, alcohol, increased doses of
multivitamins, caffeine, cigarette smoking, etc.
• Avoid self treatment – OTCs
• Support
• Assist with coping if woman has taken a teratogenic
agent..With guilt or fear…associated with drugs taken in
pregnancy.
33
34. Common Medications Safe In
Pregnancy
1.GIT conditions:
a) Nausea & vomiting:
pyridoxine with or without doxylamine,
meclizine, cyclizine, diphenhydramine
Avoid- neuroleptics , metochlorpromide (safe in
3rd trimester)
b) Constipation:
mild purgative , lubricant purgative (less safe)
Avoid- strong purgative as may cause abortion
or premature labor pain
34
35. c) Heart burn:
milk of magnesia
Avoid- anticholinergics
d) Peptic ulcer:
sucralfate, bismuthsubcitrate & H2 blockers
2.Hemopoetic
Iron, folic acid
no role of vit.B12
35
36. 3.Infections
a) Bacterial:
i. UTI
ampicillin, amoxycillin, cephalexin, cefadroxil,
cefuroxime etc.
Avoid-fluoroquinolones
ii. Other
β-lactum antibiotics (penicillin G, penicillin
V), ampicillin, amoxycillin, cloxacillin) ,
cephalosporins (cephalexim, cefadroxil,
cefuroxime, ceftriaxone) ,
macrolides(erythromycin avoid estolate salt,
azithromycin).
36
37. gentamycin & tobramycin only if serious
infection
b) Malaria:
chloroquine, quinine (higher dose may induce
labor), proguanil, pyrimethamine (with folic
acid)
c) Amoebiasis:
metronidazole, diloxanide (avoid single large
dose)
d) Worm infestations:
piperazine citrate, pyrantel pamoate,
bephenium hydroxynaphthoate, praziquintal
(teratogenic in animals not in humans)
37
38. e) Fungal infections:
miconazole, clotrimazole & nystatin
f) HIV infection:
none are safe but zidovudine and nevirapine
are given to prevent vertical transmission
g) Tuberculosis:
INH and ethambutol, if 3rd needed rifampicin,
pyrazinamide only in severe cases like
meningitis
38
39. 4. Endocrine disorders
a) Diabetes mellitus:
always use insulin
b) Hypothyroidism:
thyroxine
c) Thyrotoxicosis:
propylthiouracil
d) Corticosteroid are highly teratanogenic and
must be avoided
39
40. 5. Cardiovascular disorders
a) Hypertension:
α-methyl dopa oral & hydralazine in
emergency
β blocker like labetolol (also can be given
i.v.), atenolol
b) Thromboembolic disease:
LMWH (note just before labor)
Avoid- warfarin
40
41. 6. CNS disorders
a) General anesthetics:
thiopentone sodium & nitrous oxide
b) Headache & Inflammation:
paracetamol, codeine preparation
Avoid- other NSAIDS
aspirin can be used in lowest doses upto 2 weeks
before EDD
c) Epilepsy:
Avoid-Na valproate, phenytoin
d) Migraine:
paracetamol, propranolol, amitryptyline
41
43. 8. Others
a) Corticosteroids must be avoided except at
term for lung maturation with tocolytics
b) Fat soluble vitamins may cause subaortic
stenosis & craniofacial anomalies , so avoid
c) Vaccines: only T.T. ; avoid live vaccines
d) avoid indigenous drugs
43
45. • Most drugs are excreted into breast milk
• But they are less quantity
• Because of large volume of distribution in
mother’s body compared to small amount of
milk
• Lipophilic drugs are readily excreted also non
plasma protein bound
• pH of milk = 7.0 , slightly acidic
• Mainly transported by passive diffusion
• Adverse reaction in fetus due to
i. slower elimination ( more accumulation)
ii. Sensitive & idiosyncratic reaction
45
46. • TRH & metochlorpramide ↑es lactation
• Ergotamine & bromocriptine ↓es lactation
used in loss of fetus or newborn & in
hyperprolactinaemia
• Most of the drugs & vaccines are safe
• Drugs which are to be avoided or monitored
are discribed next
46
49. Pharmacokinetics in Children
1. Absorption
a. ↑ from skin due to thin stratum corneum & better
hydration
b. GIT: altered, low acidity, ↑ed gastric emptying time,
↑ed enterohepatic circulation, irregular
peristalsis(PCM & phenobarbitone ↓ed & of penicillin
G & ampicillin ↑ed )
c. Intramuscular & subcutaneous unpredictable
because thin skeletal muscle mass & fat
d. Low bile acid & lipase so less lipophilic drug
absorption
e. diarrhoea
49
50. 2. Drug distribution
a. More in c/o hydrophilic than adult because of
higher percentage of body water (65-85%), also
40% is extra cellular in the neonate
(aminogycoside)
b. Less fat in pre term (1% ) than full term(15%)
thus less lipophilic drug concentration in
premature
c. Less plasma protein available so more free drug ,
so more toxicity (diazepam)
d. Competition with bilirubin for albumin may
displace it , may cause kernicterus
(sulfonamides) & vice versa (phenytoin)
50
51. 3. Drug metabolism
a. Less liver cytochrome P450 dependent activity , so
chances of toxicity high e.g.chloramphenicol
causing grey baby syndrome
b. Table shows
difference in half life in
Neonate & adult
p.s.phenobarbital &
Phenytoin have low half
life during infancy
51
52. c. Enzyme induction
Due to mother receiving drugs or child
-enzyme induction may increase interaction
-phenobarbitone is used to treat neonatal
jaundice on the same principal
* During toddlerhood metabolite rate of many
drugs exceeds adult values .
52
53. 4. Drug excretion
a. GFR is less , so is tubular secretion, resulting
in less renal clearance
b. Normal clearance achieved at the age of 6-12
months
c. Subsequently during toddlerhood it increases
than adult value for some (e.g. for digoxin)
d. So appropriate dose adjustment is necessary
e. E.g. penicillin, ampicillin, aminoglycosides
53
54. Pharmacodynamic alterations
• Response of drug may be different in children
than adults but mechanism remain same
• Due to immature receptors or
neurotransmitter system
• e.g. glucocorticoids-premature epiphysial
fusion; tetracyclines- malformed bone & teeth
also staining of teeth, antihistaminics &
barbiturates –excitement, amphetamine- ↓es
abnormal hyperactivity
54
55. Clinically important
PDA can be closed with administration of
indomethacin
In case of fallot’s tetralogy administration of
alprostadil (PGE1) is life saving
55
56. Pediatric Dosage Forms & Compliance
• Use of tablets is inconvenient & injections are
rejected by children
• So preferred formulations are liquid e.g.
suspension, elixir, drops
• Proper use should be instructed
• Rejection, spitting & vomiting should be
considered
• Proper measurement
• Suspensions to be shaken well before use
• Reduce dosing errors
• Encourage children to take medicine themselves
56
57. Dose
• Young’s rule: dose= Adult dose × Age(years) /
Age + 12
• Clark’s rule: dose = Adult dose × Weight(kg) /
70
• Determination of
drug dosage from
surface area
57
59. Geriatric (>65 years) patients have more
chances of drug interactions & ADRs
1. Presence of multiple disease (avg. 5-8 drugs)
2. Sluggishness of various body functions
3. Reduced healthcare finance
4. Nutritional problem
5. Loss of spouse
6. Poor patient compliance due to poor
understanding, confusion, forgetfulness, poor
hearing, poor vision, physical disability
7. Pharmacological changes due to ageing
59
60. Pharmacokinetic Changes
a) Absorption
• Slow due to ↓ed blood flow , ↓ed motility
• Altered nutrition
• Multiple OTCs
b) Distribution
• Reduced body weight
• ↓ed body water, ↑ed body fat, ↓ed plasma
proteins
• So more free drug
60
61. c) Biotransformation
• ↓ed due to less liver mass, blood flow & reduced
ability to recover from injury so
• Phase I inactivation reduced by microsomal
mixed function oxidases
• No change in phase II reaction
• Extensively first pass metabolized drug will have
higher than normal conc. E.g. TCAs, neuroleptics,
antidysrhythmic drugs
• Less induction of hepatic microsomal enzyme so
less interaction through there
• Malnutrition & other diseases
61
62. d) Excretion
• ↓ed GFR, ↓ed tubular secretion,
• No s.creat ↑ though, due to less muscle mass
• Narrow therapeutic window drugs show
toxicity e.g. lithium, digoxin, atenolol
• Decrease respiratory capacity & more lung
diseases so less excretion through lungs e.g.
general anesthetics
• Creat cl (ml/min)= (140-Age)×(weight kg)
72 × s.creat(mg/dl)
62
63. Pharmacodynamic changes
a) Response is decreased e.g. β agonists & β blockers ,
due to ↓ed no. of receptors
b) Response is increased
• More chance of postural/orthostatic hypotension due
to reduced baroreceptor sensitivity
• Drugs acting on CNS (like sedative-hypnotics) shows
more response, more respiratory depression
• Intolerance to digitalis & neuroleptic
C) Drugs with anticholinergic activity may cause
retention in elderly with BPH
• Average BP increases
• Temperature regulation is impaired
63
64. Precautions While Prescribing To Elderly
1. Make sure of diagnosis & reuirement
2. Prescribe drug with minimal side effects
3. Prescribe minimum number of drugs (brown bag
analysis)
4. Dose adjustment to minimal & mind hepatic or
renal damage
5. Use suitable dosage form
6. Readable label , easy packing
7. ADR
8. Drug history including OTCs & herbal
64
65. 9. Use FDCs where appropriate
10. Avoid drug interactions
11. Patient compliance
12. Discontinuation of drug is as important as
starting , e.g. withdrawal syndromes, relapse
of infection
65
66. References
• Basic and clinical pharmacology by Dr. Bertram
G Katzung et al 12th edition
• A complete textbook of medical pharmacology
vol.II by Dr. S K Srivastava
• Goodman and Gilman's The Pharmacological
Basis of Therapeutics (12th Edition)
• www.cdc.gov/media/dpk/2013/docs/dpk-
safe-meds-doc1.pdf
66