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OUTLINE



DRUG INTERACTIONS - INTRODUCTION


DRUG – DRUG INTERACTIONS



FOOD – DRUG INTERACTIONS
DO WE REALLY NEED TO
STUDY DRUG
INTERACTIONS?


Meta analysis of 39 prospective clinical trials
has proved : Adverse Drug Reactions are 4th
most frequent cause of death1



Analysis of USA National Drug Register has
proved : The cause of 2/3 of ADRs are drug
interactions2

1Lazarou
2Phillips

et al: JAMA 1998
et al: JAMA 2001
DEFINITION
A

drug interaction
is a situation in
which a substance
affects the activity
of a drug, i.e. the
effects are
increased or
decreased, or they
produce a new
effect that neither
Effects of drug interaction


Drug interaction can result in
 Increased

effect – Additive or
Synergistic effect
 Increased

therapeutic effect

 Increased

toxic or adverse effect

good

bad

 Decreased

effect

effect – Antagonistic

 Decreased

therapeutic effect

 Decreased

toxic effect

bad

good
EXAMPLES


Synergistic drug-drug interaction : xanax is a drug which
belongs to benzodiazepine class of drugs ,if it is taken
along with an antidepressant like Prothiadine , the
drowsiness effect of both drugs is enhanced and
multiplied.



antagonistic drug-drug interaction : Ibuprofen enhances
salt retention by the body and the diuretic like furosemide
gets the body rid of the salt.
DIFFERENT KINDS OF DRUG
INTERACTION
PHARMACOKINETIC (PK)
Drug interactions:
PHARMACODYNAMIC (PD)


Interaction drug - drug



Interaction drug - alcohol



Interaction drug - foods (and soft drinks)



Interaction drug – food supplements

All these kinds are divided into:
Drug interactions:


clinically relevant



not clinically relevant
PHARMACOKINETIC INTERACTION





Most drug interactions involve an
alteration in the pharmacokinetics of the
drug.
Probably no ‘overlap’ in the therapeutic
effects of the two drugs.
Difficult to predict
1.

Absorption

2.

Distribution

3.

Metabolism

4.

Excretion
Drug
absorption

Transport of

the drug inside
the body

Drug
displacement
(protein-binding)

Drug metabolism
(biotransformation)
CYP3A4, CYP2D6,
CYP2C9…

Drug
excretion
Drug Absorption
 Drug

interactions can either delay the onset
of drug action or increase or decrease the
amount of drug absorbed.

 Rate

of drug absorption is a concern when a
fast onset of absorption is necessary.

 An

example of this would be analgesics. A
rapid response is often desired when the
patient is in pain.

 This

is important because it can ultimately
affect drug levels.
Distribution


When the drug leaves the systemic
circulation and moves to various parts of
the body



Drugs in the bloodstream are often
bound to plasma proteins; only
unbound drugs can leave the blood
and affect target organs



Low serum albumin can increase
availability of drugs and potentiate their
effects
Metabolism
(biotransformation)


Primarily in the liver; cytochrome P-450 enzyme
system facilitates drug metabolism; metabolism
generally changes fat soluble compounds to
water soluble compounds that can be excreted



Foods or dietary supplements that increase or
inhibit these enzyme systems can change the
rate or extent of drug metabolism
Excretion
• Drug interactions that involve
excretion can affect the amount
of drug that is either secreted or
reabsorbed.
• Some strong acids/bases are actively
secreted/reabsorbed by renal tubules.
• Digoxin excretion may be reduced by
verapamil and quinidine.Some drugs sensitive
to changes in urinary pH or sodium balance.
Pharmacodynamic
mechanisms


Two drugs acting upon the same (or similar)
mechanism in the same ‘direction’ (i.e. two
agonists).
 E.g.

Two beta-blockers additive
 E.g. Morphine plus diazepam additive
 E.g.



Pen-G plus gentamicin synergistic

Two drugs acting upon the same (or similar)
mechanism in opposite ‘directions’ (i.e.
agonist plus antagonist).
 E.g.

Beta-blocker plus salbutamol antagonistic
 E.g. Frusemide plus NSAID indirectly antagonistic
Probability of drug interaction

risk of drug interaction

60%
50%
40%
30%
20%
10%
0%
2

5

10

15

20

number of drugs used

Probability of drug interaction rises with the
number of drugs patient uses
More drug = More interactions
Drug Interactions: A Comprehensive Guide

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Drug Interactions: A Comprehensive Guide

  • 1.
  • 2. OUTLINE  DRUG INTERACTIONS - INTRODUCTION  DRUG – DRUG INTERACTIONS  FOOD – DRUG INTERACTIONS
  • 3. DO WE REALLY NEED TO STUDY DRUG INTERACTIONS?
  • 4.  Meta analysis of 39 prospective clinical trials has proved : Adverse Drug Reactions are 4th most frequent cause of death1  Analysis of USA National Drug Register has proved : The cause of 2/3 of ADRs are drug interactions2 1Lazarou 2Phillips et al: JAMA 1998 et al: JAMA 2001
  • 5. DEFINITION A drug interaction is a situation in which a substance affects the activity of a drug, i.e. the effects are increased or decreased, or they produce a new effect that neither
  • 6. Effects of drug interaction  Drug interaction can result in  Increased effect – Additive or Synergistic effect  Increased therapeutic effect  Increased toxic or adverse effect good bad  Decreased effect effect – Antagonistic  Decreased therapeutic effect  Decreased toxic effect bad good
  • 7. EXAMPLES  Synergistic drug-drug interaction : xanax is a drug which belongs to benzodiazepine class of drugs ,if it is taken along with an antidepressant like Prothiadine , the drowsiness effect of both drugs is enhanced and multiplied.  antagonistic drug-drug interaction : Ibuprofen enhances salt retention by the body and the diuretic like furosemide gets the body rid of the salt.
  • 8.
  • 9. DIFFERENT KINDS OF DRUG INTERACTION PHARMACOKINETIC (PK) Drug interactions: PHARMACODYNAMIC (PD)  Interaction drug - drug  Interaction drug - alcohol  Interaction drug - foods (and soft drinks)  Interaction drug – food supplements All these kinds are divided into: Drug interactions:  clinically relevant  not clinically relevant
  • 10.
  • 11. PHARMACOKINETIC INTERACTION    Most drug interactions involve an alteration in the pharmacokinetics of the drug. Probably no ‘overlap’ in the therapeutic effects of the two drugs. Difficult to predict 1. Absorption 2. Distribution 3. Metabolism 4. Excretion
  • 12. Drug absorption Transport of the drug inside the body Drug displacement (protein-binding) Drug metabolism (biotransformation) CYP3A4, CYP2D6, CYP2C9… Drug excretion
  • 13. Drug Absorption  Drug interactions can either delay the onset of drug action or increase or decrease the amount of drug absorbed.  Rate of drug absorption is a concern when a fast onset of absorption is necessary.  An example of this would be analgesics. A rapid response is often desired when the patient is in pain.  This is important because it can ultimately affect drug levels.
  • 14.
  • 15. Distribution  When the drug leaves the systemic circulation and moves to various parts of the body  Drugs in the bloodstream are often bound to plasma proteins; only unbound drugs can leave the blood and affect target organs  Low serum albumin can increase availability of drugs and potentiate their effects
  • 16. Metabolism (biotransformation)  Primarily in the liver; cytochrome P-450 enzyme system facilitates drug metabolism; metabolism generally changes fat soluble compounds to water soluble compounds that can be excreted  Foods or dietary supplements that increase or inhibit these enzyme systems can change the rate or extent of drug metabolism
  • 17. Excretion • Drug interactions that involve excretion can affect the amount of drug that is either secreted or reabsorbed. • Some strong acids/bases are actively secreted/reabsorbed by renal tubules. • Digoxin excretion may be reduced by verapamil and quinidine.Some drugs sensitive to changes in urinary pH or sodium balance.
  • 18. Pharmacodynamic mechanisms  Two drugs acting upon the same (or similar) mechanism in the same ‘direction’ (i.e. two agonists).  E.g. Two beta-blockers additive  E.g. Morphine plus diazepam additive  E.g.  Pen-G plus gentamicin synergistic Two drugs acting upon the same (or similar) mechanism in opposite ‘directions’ (i.e. agonist plus antagonist).  E.g. Beta-blocker plus salbutamol antagonistic  E.g. Frusemide plus NSAID indirectly antagonistic
  • 19. Probability of drug interaction risk of drug interaction 60% 50% 40% 30% 20% 10% 0% 2 5 10 15 20 number of drugs used Probability of drug interaction rises with the number of drugs patient uses
  • 20. More drug = More interactions