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Oral contraceptive prescribing

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Oral contraceptive prescribing. clinical pharmacology. mechanism of action ... concentrations (eg rifampicin, griseofulvin, anticonvulsants, St John's Wort) ... – PowerPoint PPT presentation

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Title: Oral contraceptive prescribing


1
Oral contraceptive prescribing
2
  • clinical pharmacology
  • mechanism of action
  • ADME
  • interactions
  • adverse reactions
  • benefits and harms

3
what are they
  • around since late 1950s
  • social revolution
  • progestogen /oestrogen
  • variety of components and doses
  • changes over time in both

4
components
  • oestrogen
  • ethinyoestradiol
  • mestranol
  • progestogen
  • norethisterone
  • norgestrel
  • Levonorgestrel
  • medroxyprogesterone
  • ethynodiol diacetate
  • gestodene
  • desogestrel

5
doses
  • monophasic
  • oestrogen - up to 50?g/day
  • progestogen - up to 1mg/day
  • biphasic
  • oestrogen constant
  • progestogen eg 11 days _at_50, 10 _at_125 ?g
  • triphasic
  • oestrogen 30/40/30
  • progestogen 50/75/125

6
clinical pharmacology
  • mechanism of action
  • inhibit secretion of FSH, LH - inhibit ovulation
  • additional actions on endometrium tubal motility,
    cervical mucosa

7
clinical pharmacology
  • absorption
  • well absorbed orally
  • distribution
  • bound to plasma proteins
  • albumin, SBG, others

8
metabolism
  • Oestrogens
  • first pass clearance
  • metabolised in liver, conjugated
  • excreted in the bile - (estradiol vs EE)
  • enterohepatic circulation
  • Progestogens
  • depends on which one - natural progestogen
    extensive first pass metabolism

9
excretion
  • urinary
  • remember the bile duct

STO
HV
PV
CBD
About 40-60 of estrogen removed in the first
pass through the liver HMW conjugates are
excreted in bile
10
interactions (1)
  • antibiotics
  • impaired absorption (effect on gut enzymes)
    reduced bacterial sulfatase leading to reduced
    entero-hepatic recycling
  • enzyme induction -gt increased clearance, lower
    plasma estrogen concentrations (eg rifampicin,
    griseofulvin, anticonvulsants, St Johns Wort)

11
interactions (2)
  • anticonvulsants
  • Older drugs are enzyme inducers -gt increased
    clearance and reduced concentration and failure
    (phenytoin, phenobarbitone, primidone,
    carbamazepine). No effect of sodium valproate
  • Newer drug have variable effects (no change with
    gabapentin, lamotrigine, tiagabine,
    levetiracetam) (induction with topiramate and
    oxcarbazepine)
  • try higher dose estrogen pills, double product
    dosing
  • valproate less of a problem

12
adverse reactions
  • estrogen excess
  • late cycle breakthrough bleeding
  • menorrhagia/dysmenorrhoea
  • nausea/vomiting
  • fluid retention
  • breast tenderness

13
adverse reactions
  • progestogen excess
  • amenorrhoea
  • acne/oily skin
  • weight gain
  • mood changes
  • depressed libido
  • breast tenderness

14
other risks
  • thromboembolic disorder
  • high dose oestrogen - Inman, dose response
    relationship
  • worse with other risk factors (age, smoking)
  • ?third generation progestogens
  • differentiating effects on VTE and other
    cardiovascular disease

15
big picture risks
  • endometrial cancer
  • progestogen is protective
  • ovarian cancer
  • protective
  • breast cancer
  • jury out /data unconvincing
  • cervical cancer
  • confounded

16
other benefits
  • reduction in menstrual flow - may lower incidence
    of anemia
  • reduction in dysmenorrhoea
  • possible reduction in auto-immune thyroid
    disease, rheumatoid arthritis
  • some protection against PID

17
risk of nonfatal VTE
18
other issues
  • compliance
  • gastro.
  • missing pills
  • alternative forms of hormonal contraception

19
balance sheet
  • benefits
  • effective contraception
  • other health benefits
  • long-term health and social impact
  • harms
  • immediate adverse effects
  • risk of failure
  • long-term health effects

20
other uses
  • morning after pill
  • EE 100mcg norgestrel 1mg within 72 hours, 2
    doses
  • Failure rate of about 1
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